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VOLUME 38 NUMBER 4
DECEMBER 2006
KMJ
KMJ
KUWAIT MEDICAL JOURNAL
The Official Journal of The Kuwait Medical Association
EDITORIAL
Science Versus Scientism
263
Belle M Hegde
REVIEW ARTICLE
Plant-derived Health-effects of Turmeric and Curcomenoids
267
Stig Bengmark
ORIGINAL ARTICLES
Feasiblity and Clinical Significance of Echocardiographic Assessment of Aortic Root Compliance in
Hypertensive Patients
276
Aly Mohamad Hegazy, Laila Soud M Al-Einzi, Mohamad Hussain Al-Kandari, Bader Abdelkader
Prevalence and Factors Associated with Obesity and Treatment of Blood Pressure among Kuwaiti
Hypertensive Patients in a Primary Health Care Clinic
284
Nadia Yousef Al-Mahmoud
Factors Influencing Outcome of Congential Diaphragmatic Hernia
287
Bhaskar Gupta
Anomalous Coronary Artery from the Opposite Coronary Sinus in Young Children
292
Mustafa A Al-Qbandi, Jeffrey Smallhorn
Results of Combined Proximal Crescentic Metatarsal Osteotomy and Modified Distal Soft Tissue
Procedure in Severe Hallux Valgus
300
Ibrahim MAAl-Kussary, Fathy Khallaf, Mahmoud El Rayes, Mustafa Al Akkad
Safety of Laparoscopy in Acute Cholecystitis
308
Wael Fathi Hassaniah, Mohamed Al Haifi, Talib Jumaa
INSIGHT
Computerization in Primary Care: an Insight
311
Huda I Al-Shaibani, Siham YF Al-AbdulGhafour, Amal H Al-Saqabi
CASE REPORTS
Neuronal Ceroid Lipofuscinoses: Report of Five Cases in Kuwait
315
Maliha Askar Soud Al-Bloushi , Jehoram T Anim , Yousif Kasim Habeeb
Adrenal Carcinoma with Cardiac Metastasis in a Child: Case Report
321
Abdelmohsen Ben-Nakhi, Ali Hussain, Khaledah Dashti
Excision of Ventricular Cysts of Larynx using Zero Degree and 30 Degree Endoscope
324
Pradeep Shenoy, Sohail Abdul Malik, Rashid Al Duwillah
Sickle Cell Intra-Hepatic Cholestasis : A Rare but Fatal Disease
326
Saad AL-Zanki, Moza AL-Saleh
Carbamezepine Induced Pseudolymphoma
329
Shahid Aziz, Abdulkarim Al Aska, Ayman M Al Kharabah
Walker-Warburg Syndrome, A Case Report
332
Magdy H Shafik, Mohamed Taha Mohamed, Talaat M Yousef
KU ISSN 0023-5776
Continued inside
Vol. 38 No. 4
THE KUWAIT MEDICAL JOURNAL
December
December2006
2006
KUWAIT MEDICAL JOURNAL
C O N T E N T S
Continued from cover
SELECTED ABSTRACTS OF ARTICLES PUBLISHED ELSEWHERE BY
AUTHORS IN KUWAIT
336
FORTHCOMING CONFERENCES AND MEETINGS
339
WHO-FACTS SHEET
344
1. New Global Estimates to Mark World Sight Day
2. A Clean Bill for Indoor Use of DDT to Control Malaria
3. Emergence of XDR-TB
4. Call for Intensified Action to Halt a Quarter of a Million Tb/Hiv Deaths a Year
5. Helmet Use Saves Lives
ARABIC ABSTRACTS OF ARTICLES PUBLISHED IN THIS ISSUE
349
YEARLY AUTHOR INDEX - KUWAIT MEDICAL JOURNAL (KMJ) 2006;
VOLUME 38
353
YEARLY TITLE INDEX - KUWAIT MEDICAL JOURNAL (KMJ) 2006;
VOLUME 38
355
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KMJ
Kuwait Medical Journal (KMJ)
Published by the Kuwait Medical Association
Previously known as The Journal of the Kuwait Medical Association (Est. 1967)
Honorary President: Abdulaziz Al-Babtain
EDITORIAL BOARD
Editor-in-Chief:
Editor:
International Editor:
Associate Editors:
Circulation Manager:
Fuad Abdulla M Hasan
Adel Khader Ayed
Pawan K Singal
Adel A Alzayed
Mousa Khoursheed
Mustafa M Ridha
Nasser Behbehani
Homoud Fahad Al-Zuabi
INTERNATIONAL ADVISORY BOARD
Allan Templeton, UK
Ananda S Prasad, USA
Anders Lindstrand, Sweden
Andrew J Rees, UK
Arie van Dalen, Netherlands
Belle M Hegde, India
Bengt Jeppsson, Sweden
Charles A Dinarello, USA
Christian Imielinski, Poland
Elizabeth Dean, Canada
Fiona J Gilbert, UK
Frank D Johnston, UK
Gabrielle M Hawksworth, UK
George Russell, UK
Graeme RD Catto, UK
Jan T Christenson, Switzerland
Jaroslav Slipka, Czech Rep
Jasbir S Bajaj, India
John V Forester, UK
Julian Little, Canada
Lubomir Karagiosov, Bulgaria
Lewis D Ritchie, UK
Neva E Haites, UK
Nirmal K Ganguli, India
Oleg Eremin, UK
Peter JB Helms, UK
Peter RF Bell, UK
Raymond M Kirk, UK
S Muralidharan, India
Tulsi D Chugh, India
William ATweed, Canada
William B Greenough, USA
Zoheir Bshouty, Canada
REGIONAL ADVISORY BOARD
Abdulla Behbehani
Abdul Mohsen Jaffar
Abeer K Al-Baho
Alexander E Omu
Ali Al-Mukaimi
Ali Al-Sayegh
Asmahan Al-Shubaili
Chacko Mathew
Eiman M Mokaddas
Faisal A Al-Kandari
Habib Abul
Hilal Al-Sayer
Jasbir Singh Juggi
John F Greally
Joseph C Longenecker
Kamal Al-Shoumer
Kefaya AM Abdulmalek
Khalid Al-Jarallah
Marie T Greally
Mazen Al Essa
Mohamed AA Moussa
Mohammed Al-Jarallah
Mousa Khadadah
Mubarak Al-Ajmi
Mustafa Al-Mousawi
Nasser J Hayat
Nebojsa Rajacic
Sadika Al-Awadi
Saleema Al-Ramadan
Sami Asfar
Soad Al-Bahar
Sukhbir Singh Uppal
Waleed Alazmi
ARABIC TRANSLATION: Arabization Centre for Medical Science (ACMLS), Kuwait
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KUWAIT MEDICAL JOURNAL
KUWAIT MEDICAL JOURNAL (KMJ)
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Instructions for Authors
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EXAMPLES
Article
Burrows B, Lebowitz MD. The β agonists
dilemma (editorial). N Engl J Med 1992; 326:560-561.
Book
Roberts NK. The cardiac conducting system and
His bundle electrogram. New York, AppletonCentury-Crofts, 1981: 49-56.
ii
KUWAIT MEDICAL JOURNAL
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Book chapter
Philips SJ, Whisnam JP. Hypertension and
stroke. In: Laragh JH, Bremner BM, editors.
Hypertension: pathophysiology, diagnosis, and
management. 2nd ed. New York: Raven Press; 1995,
p 465-478.
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Kuwait Medical Journal
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iii
Instructions for Authors
December 2006
KUWAIT MEDICAL JOURNAL
Editorial
Science Versus Scientism
Belle M Hegde
The Middlesex Hospital Medical School, University of London, UK
Northern Colorado University, USA,
Indian Institute of Advanced Studies, Shimla, India
MAHE University, Manipal, India
Kuwait Medical Journal 2006, 38 (4): 263-266
“The central problem of our age is how to act
decisively in the absence of certainity.”
Bertrand Russell
Science and scientific temper simply mean
curiosity. They are efforts to get to know the secrets
of Nature. Many a time, Nature refuses to fully
divulge her secrets when one goes very close.
Children, before they start schooling are curious,
but when they come out they become, by and large,
just repetitive robots because of their brainwashing
in schools about the accepted norms in science.
Occasionally, there are exceptions, but their
numbers are very small. To swim against the
current is not easy, either. Research depends on
grant money; most grants come either from the
government or industry. Both masters would like
their interests guarded. Refutative research, which
tries to demolish the scientific myths, is not funded
and so is nipped in the bud. Publishing the data
from those studies is almost impossible in the
present atmosphere[1]. Even one’s position in a
University might be threatened!
Scientism, on the contrary, is like a powerful
religion that tries to influence people’s understanding
of this Universe in the accepted norms. Any attempt
to show evidence to the contrary is being hushed
up with all the might at their command. Scientism
was helped by the early successes of technology
based on the present scientific paradigm. Society
venerates science for the simple reason that we
have the telephone, electricity, easy transportation,
satellites, space ships, nuclear war heads and the
computers et cetera, thanks to the conventional
scientific paradigm. In addition, there is this big
money business in scientific technology. Powerful
countries are sold to scientism because they have
been able to build destructive weapons, thanks to
scientism. These weapons give the countries
enormous powers to dominate the world. The lure
of medals and prizes and the large amount of
money involved in some of the prizes like the
Nobel have even made people fake research
findings or plagiarize them from others without
acknowledging the original source[2].
That is how science got a clean chit from society.
Let us examine the present strong pillars of science
to see how strong and solid they are. The Big Bang,
origin and evolution of the human species, the
relativity theory and, quantum mechanics are those
four pillars[3]. Reductionism and statistics are the
pillars of medical science and biology[4]. Darwin’s
theory of evolution is found wanting in many areas.
Evolution inside a species is different from evolution of a
new species; a bird from a fish, for example. The latter
needs thousands of biochemical reactions that
individually will have no survival advantage when
the ultimate new species arrives by accident[5]. The
efforts by Richard Dawkins to sell Darwinism to the
public are not very scientific either. One example of
the very complicated eye developing from a small
depression in the earlier species looks rather too
simplistic[6].
The relativity theory, first developed by a
German physicist, Lorenz along with the French
mathematician, Poincare, had a significant contribution
also from the famous Irish mathematician,
Fitzgerald[7]. Albert Einstein, the deified guru of
physics, had very little to do with it. Einstein,
however, had contributed immensely to Brownian
movement, photoelectric effect and movement of
ions in solutions[8]. Einstein giving away his Nobel
Prize money to his first wife, whom he had
divorced by then, gives credence to the view, held
by some close confidents, that the original Nobel
paper of Einstein did have his wife’s name as the
first author, which must have disappeared later [9].
Be that as it may, the question raised by
Professor Dingle of the London University about
the theory remains unanswered so far [10]. The
assumption in the theory that there is same velocity
of light independent of the direction of measurement
Address Correspondence to:
Prof. B. M. Hegde, MD, FRCP, FRCPE, FRCPG, FRCPI, FACC, FAMS, “Manjunath” Pais Hills, Bejai, Mangalore-575004, India. Tel: +91 824
245 0450. E-mail: [email protected], web site: www.bmhegde.com
264
with respect to the motion of the earth has recently
been found to be inconsistent[11]. The jewel in the
crown of physics, the quantum theory, does not
seem to have much connection to reality. We still do
not have answers to questions like a) what is a
wave function, b) In the Schrödinger’s equation
what are the waves “of” and what are the waves
“in”, and third c) what is an electron[12].
The basic problem in the theory of evolution
would be, if we accept that there is no design and
there is no teleology as sold by the scientific
establishment, to explain the prior existence of the
DNA! The accepted laws of chemistry need chance
collisions between simpler constituents[13]. Darwin’s
book Descent of Man makes it mandatory for us to
discount any design. Dawkin’s book The Blind
Watchmaker makes an effort to whitewash these
questions![14] Lamarck must have had his last laugh
in his grave when he came to know that rats
developed diabetes following destruction of their
pancreas by drugs: they then passed the disease on
to their offsprings - evolution through inheritance
of acquired characteristics - Lamarckism[15]. One
would benefit a lot by understanding the word
Entelechy - spontaneous development of order, as
opposed to entropy - disorder, first coined by the
German biologist, Driesch (1867-1941) [16].
NASA claims that there is no life anywhere
outside the Earth, but they could not discount
bacterial life deep down the surface of Mars. There
are some indicators to that possibility in the recent
works. Mathematics, the foundation of all sciences,
including the King of sciences, physics, cannot
explain many of our experiences in life. Let me
quote Albert Einstein himself here: “Insofar as the
propositions of mathematics give an account of
reality, they are not certain; and insofar as they are
certain, they do not describe reality”[17]. If there is no
design, how could a high school student, Ramanujam,
write down large number of new and original
theorems, some of which he could prove but, some
others he simply stated as true, and were later
proved by other mathematicians at the Cambridge
University?[18].
The remarkable picture of that gigantic explosion,
the Big Bang that began the Universe: the latter
expanding ever since, is understood even by a
school boy/girl. What happened before the Big
Bang?[19]. Maddox, the then editor of Nature, in 1989
did write that Big Bang theory would be forgotten
by 2000 AD. Edwin Hubble did put forward
arguments against the theory but the big one bangs
on![20]. The Tired Light hypothesis shows that the
Universe is not expanding. All that we can say
about the universe today is that it is very, very old.
December 2006
The million dollar question as to how the world
began remains unanswered![21]. Big bang and the
Black holes make good material for lay books that
are sold like hot cakes and make their authors very
rich, but most of that stuff is still in the realm of
science fiction![22, 23].
Science deals with our five senses only. What the
senses cannot measure and observe does not make
science in the present paradigm. However, the
observers’ consciousness impinges on the findings.
An electron is what it is depending on who looks at
it! When no one is looking at the electron, no one
knows what the electron does![24, 25]. There are a lot of
things in this universe that our five senses cannot
realize and they exist all the same. Science does
accept that what is known today could be proven
wrong or replaced by a new theory tomorrow, but
to say that what we don’t know today (or what
does not fit into the present paradigm) is
unscientific is illogical. But that is exactly what
scientism is trying to do.
To give a few day-to-day examples: we are not
able to measure our thoughts, our emotions, and
many of our actions based on those emotions and
thoughts. Do they, then, fall out side the realm of
science? Do thoughts exist? Do emotions have any
role in human physiology?[26]. If the answer is yes,
then we need a change of paradigm in science, at
least in medical science, where the RCTs (randomized
controlled studies) have been sold as the last word
in medical research. The truth is that there is
everything wrong with this approach. No two
human beings could be compared based on a few of
their phenotypical features. The results are there for
all to see. Most, if not all, RCTs have given unreliable
results in the long run. But look at the following in
the encyclopedia of RCTs published by the
establishment!
“A major difficulty in dealing with trial results
comes from commercial, political and/or academic
pressure. Most trials are expensive to run, and will
be the result of significant previous research, which
is itself not cheap. There may be a political issue at
stake (cf. MMR vaccine) or vested interests (cf.
homoeopathy). In such cases there is great pressure
to interpret results in a way which suits the viewer,
and great care must be taken by researchers to
maintain emphasis on clinical facts.
Most studies start with a ‘null hypothesis’ which
is being tested (usually along the lines of ‘Our new
treatment x cures as many patients as existing
treatment y’) and an alternative hypothesis (‘x
cures more patients than y’). The analysis at the end
will give a statistical likelihood, based on the facts,
of whether the null hypothesis can be safely
December 2006
KUWAIT MEDICAL JOURNAL
rejected (saying that the new treatment does, in
fact, result in more cures). Nevertheless this is only
a statistical likelihood, so false negatives and
false positives are possible. These are generally set
at an acceptable level (e.g., 1% chance that it was a
false result). However, this risk is cumulative.
There is a tendency for these two to be seized on
by those who need that proof for their point of
view.”[27].
Before we do more damage to mankind by
blindly following the reductionist paradigm, at
least in medical sciences, let us think of a new
paradigm.
Let research be directed to find out the myths
and dogmas in the present paradigm and to replace
them with newer ideas and findings that might
make life easier for mankind. Of course, it might
destroy our “rice bowl” for the moment, but we
might get a bigger bowl in future. Scientific temper
should make us identify the false dogmas and
enable us to destroy them. Science is change and
what does not change is not science. Professor John
O’M Bockris so beautifully describes the new
paradigm shift that is needed in science in his
classic The New Paradigm[3]. What does not change
becomes religion. That is why I sometimes feel, that
scientism is a kind of religion we are made to follow
blindly. Present science is excited about nanobots
but does not bother about our giga problems like
environmental pollution, abject poverty of the
majority, preventable illnesses which kill the poor
and unemployment of the majority!
It is preposterous that medical science does not
worry about health promotion, while it goes
overboard about disease interventions, many of
which make the patient worse! Sir William Osler
had warned us not to intervene when the patient is
doing well, but that is exactly what we do today!
Medicine does not believe in the wellness concept.
Everyone is ill unless proved otherwise is the
present paradigm, thanks to the total body
scanners. Routine check up is the biggest medical
industry, while we know that predicting the future
is impossible in a dynamic human system using a
few data of the initial state. Even changing those
parameters might not hold good as time evolves[28].
Changing those parameters might even harm
patients in the long run, while it is mandatory to do
so, if the patient is syptomatic and is suffering,
because doctors are here to “cure rarely, comfort
mostly but to console always.”
The effort here is not to belittle the great strides
science has made in the last two centuries. The
stress here is to let the reader know that there is so
much noise in this area that almost drowns the
signal! Unless we silence those noises and try to pick
265
the signals, science will not progress and mankind
will still be in the dark[29, 30] . Even if one person is
stimulated to think on those lines, the purpose of
writing this will have been achieved, despite the
fact that 99% of the readers would be angry or
unhappy about the contents. Conventional journals
would hesitate to publish this piece for obvious
reasons - their peer reviewers will not permit it and
the editors dare not take the responsibility
themselves!
“Certainty generally is illusion and repose is
not the destiny of mankind.”
Oliver Wendell Holmes Jr
ACKNOWLEDGMENT
I remain ever grateful to Professor John O’M
Bockris, Distinguished Professor and Head of
Chemistry at Texas A&M University, for I have
drawn very liberally from his classic The New
Paradigm, published by A and M Enterprises
Publishers, College Street, Texas in 2005, for this
article.
REFERENCES
1.
2.
3.
4.
5.
6.
7.
8.
9.
10.
11.
12.
13.
14.
15.
16.
17.
Hegde BM. Need for a change in medical paradigm. Proc
Royal Coll Physi Edinb 1993; 23: 9-12.
Campbell EG, Louis KS, Blumenthal D. Looking a gift horse
in the mouth. JAMA1999; 279: 995-999.
Bockris J O’M. The New Paradigm. A&M Publishers,
College Street, Texas. 2005.
Milloy S. Science without Sense. Cato Institute, 1997,
Washington DC.
Behe MJ. Darwin’s Black Box. Free Press, New York, 1996
Dawkins R. The Blind Watchmaker. WW Norton and Co.
1996.
Poincare JH. Relativity theory before Einstein. Arch
Netherlands Sci 1900; 2: 232.
Hey T and Walters P. Einstein’s Mirror. Cambridge
University Press, 1997.
Bjerknes C. Einstein as a plagiarist. XTX Corp. Downess
Grove, IL. 2002.
Dingle H. Science at the cross roads - Doubting relativity.
Martin and O’Keefe. London, 1972. (also, Dingle’s
unanswered question. Nature August 31, 1973).
Michelson AAand Morley EW. Velocity of light in various
directions compared to the direction of movement of the
earth. Am J Sci 1887; 3: 333.
Lindley D. Where does the quantum weirdness go? Basic
Books 1996.
Steinman G and Cole MN. Synthesis of biologically
pertinent peptides under possible primordial conditions.
Proceedings National Academy of Sciences of USA, 1967.
Milton R. Shattering the myth of Darwinism Park Street
Press, 1997.
Lamarque JR. Natural History. Daterville, 1815, Paris.
Freyhofer HH. The vitalism of Hans Driesch: The success
and decline of a scientific theory. Peter Lang Publishing.
1982.
Hey T and Walters P. Einstein’s Mirror. Cambridge
University Press. 1997.
266
Science Versus Scientism
18. Kanigel R. The Man who knew Infinity- A life of the genius
Ramanujam. Washington Square Press, April 1991.
19. Lorenz H, Mie G. In: Paula La Violette, Beyond the Big
Bang. Park Street Press: Rochester; Vermont, 1995.
20. Tully RB. Origin of the Hubble Constant Controversy.
Nature 1988; 334: 209.
21. Lerner E. The Big Bang never happened! Vintage Books.
1991.
22. Hawking S. A Brief History of Time. Bantum Books, 2000.
23. Weinberg S. The First Three Minutes. Basic Books, New
York, 1997.
24. Schrödinger E. Science and Humanism, Cambridge
December 2006
University Press. 1954.
25. Wigner EP. Consciousness affects wave function. In: The
Scientist Speculates (ed. Good IT) Heinemann, London,
1961.
26. Penrose R. Shadows of the mind. Oxford University Press.
1994
27. Randomized controlled trial -www. wikipedia.org/wiki/
randomised controlled trials.
28. Firth WJ. Chaos - predicting the unpredictable. BMJ 1991;
303:1565-1568.
29. Pratt D. Consciousness, Causality, and new Physics. Soc Sci
Explorer 1979; 11: 67-78.
30. Kaul. PN. Mind over Matter. The Scientist 2003; 17: 8.
December 2006
KUWAIT MEDICAL JOURNAL
Review Article
Plant-derived Health-Effects of Turmeric and Curcumenoids
Stig Bengmark
Lund University, Lund, Sweden
London University, Departments of Hepatology and Surgery, Institute of Hepatology, University College, London Medical
School, United Kingdom
Kuwait Medical Journal 2006, 38 (4): 267-275
ABSTRACT
The world suffers an epidemic of both critical (CI) and
chronic illnesses (ChDs), and both increase from year to
year, and have done so for several decades. It is strongly
associated to modern, so called Western, life style: stress,
lack of exercise, abuse of tobacco and alcohol, and to the
transition from natural unprocessed foods to processed,
calorie-condensed and heat-treated foods. There is a
strong association between ChDs and reduced intake of
plant fibres, plant antioxidants and increased consumption
of industrially produced and processed products
especially dairy, refined sugar and starch products.
Heating up foods such as milk (pasteurization), and
production of and storage of milk powder, produces
AN EPIDEMIC OF CHRONIC DISEASES AND
CRITICAL ILLNESS
Modern medicine has to a large extent failed in
its ambition to control both acute and chronic
diseases. In acute diseases; those defined as
medical and surgical emergencies such as
myocardial infarction, stroke and severe pancreatitis,
and those related to advanced medical and surgical
treatments, such as stem cell transplantation or
advanced surgical operations, there is an unacceptably
high morbidity and co-morbidity. Furthermore, the
world suffers an epidemy of chronic diseases of a
dimension never seen before, and these diseases are
now like a prairie fire also spreading to so-called
developing countries. Chronic diseases - including
diseases such as cardiovascular and neurodegenerative
conditions, diabetes, stroke, cancers and respiratory
diseases - constitute 46% of the global disease
burden and 59% of the global deaths today; each
year on earth, approximately (app) 35 million
individuals will die in conditions related to chronic
diseases, and the numbers are increasing and have
done so for several years [1]. Similarly, the morbidity
related to advanced medical and surgical treatments
and emergencies, especially infectious complications,
is also fast increasing. Sepsis is the most common
medical and surgical complication, estimated only
large amounts of advanced glycation products (AGEs)
and advanced lipoxidation products (ALEs), known as
potent inducers of inflammation. Numerous plantderived, but also microbe-derived, substances, often
referred to as chemopreventive agents, have documented
anti-inflammatory effects and are believed to reduce
speed of aging, prevent degenerative malfunctions of
organs and development of acute and chronic diseases.
Among them are various curcumenoids found in
turmeric curry foods and, thousands more of hitherto
less or unexplored substances. This review focuses on
documented experimental and clinical effects of
supplementation of turmeric, various curcumenoids and
pure curcumin.
in the US to annually affect as many as 751,000[2,3],
and cause the death of app 215, 000 patients (29%)[3].
This makes sepsis the tenth most common cause of
death in the country. It is especially alarming that
both morbidity and mortality in critical illness (CI),
especially when septic, is fast increasing and has
done so for several decades. With a documented
1.5% rate of increase per year it might double
within the coming 50 to 60 years.
LIFE-STYLE ASSOCIATED DISEASES
Accumulating evidence supports the association
of ChDs to modern life style, stress, lack of exercise,
abuse of tobacco and alcohol, and to the transition
from natural unprocessed foods to processed,
calorie-condensed and heat-treated foods. There is
a strong association between ChD and reduced
intake of plant fibres, plant antioxidants and
increased consumption of industrially produced and
processed dairy products, refined sugars and starch
products. The per capita consumption of refined
sugar has increased from about 0.5 kg per person
per year in 1850 to almost 50 kg/person/year in the
year 2000 and the per cow milk production from 2
to 50 liters/day. Dairy products, especially milk
(mostly from pregnant cows) are rich in proinflammatory molecules: hormones such as
Address correspondence to:
Stig Bengmark, MD, PhD, FRACS (hon), FRCPS (hon),185 Barrier Point Road, Royal Docks, London, E16 2SE, United Kingdom. Tel & Fax:
+44 20 7511 6842. E-mail: [email protected]
268
Plant-derived Health-Effects of Turmeric and Curcomenoids
estrogens and growth factors such as IGF-1.
Consumption of bovine milk has also been shown
to release inflammatory mediators, increase intestinal
permeability and induce leakage of larger
molecules such as albumin and hyaluronan into the
body. Heating up milk (pasteurization), and
especially production of and storage of milk
powder, produces large amounts of advanced
glycation products (AGEs) and advanced lipoxidation
products (ALEs)[4], known as potent inducers of
inflammation. This information is especially
important as many foods such as icecream, enteral
nutrition solutions and baby formulas are based on
milk powder. Bread, especially from glutencontaining grains, is also rich in molecules with
documented pro-inflammatory effects, and bread
crust is often used experimentally to induce
inflammation (See further Bengmark) [5-7].
PLANT-DERIVED PROTECTION
Common to those suffering from ChD as well as
CI is that they suffer an increased degree of
inflammation, most likely due to their Western
lifestyle. We are increasingly aware that plantderived substances, often referred to as chemopreventive agents, have an important role to play in
the control of inflammation. These substances are
not only inexpensive, they are also easy available,
and have no or limited toxicity. Among these
numerous chemo-preventive agents are a whole
series of phenolic and other compounds believed to
reduce speed of aging and prevent degenerative
malfunctions of organs, among them various
curcumenoids found in turmeric curry foods and,
thousands more of hitherto less or unexplored
substances. However, this review will mainly focus
on curcumin and its effects.
Polyphenols have in the recent few years
received increasing attention for their strong
chemo-preventive ability. Curcumin and many
other plant-derived substances are increasingly
regarded as shields against disease. Curcumin is
the most explored of the so called curmenoids, a
family of chemo-preventive substances present in
the spice turmeric. Although the substance has
been known for some time, it is in the most recent
years that the interest has exploded, much in
parallel with increasing concern for severe sideeffects of synthetic COX-2 inhibitors, marketed by
pharmaceutical industry. Most of the reported
curcumin studies in the literature are experimental
and few clinical studies are thus far presented.
CURCUMIN - AN ANTIOXIDANT AND
INHIBITOR OF NF- KB, COX-2, LOX AND INOS
NF-KB plays a critical role in several signal
December 2006
transduction pathways involved in chronic
inflammatory diseases [8] such as asthma and
arthritis and various cancers[9]. Activation of NF-KB
is linked with apoptotic cell death; either
promoting or inhibiting apoptosis, depending on
cell type and condition. The expression of several
genes such as cyclo-oxygenase-2 (COX-2), matrix
metaloproteinase-9 (MMP-9), inducible nitric oxide
synthase (iNOS), tumor necrosis factor (TNF),
interleukin-8 (IL-8), eotaxin, cell surface adhesion
molecules and anti-apoptotic proteins are regulated
by NF- KB[10]. COX-2 is inducible and barely
detectable under normal physiological conditions,
but is rapidly, but transiently, induced as an early
response to pro-inflammatory mediators and
mitogenic stimuli including cytokines, endotoxins,
growth factors, oncogenes and phorbol esters.
COX-2 synthesizes series-2 prostaglandins (PGE2,
PGF2-α), which contribute to inflammation,
swelling and pain. PGE2 promotes production of
IL-10, a potent immuno-suppressive cytokine
produced especially by lymphocytes and macrophages,
and suppression of IL-12[11]. Inducible nitric oxid
synthase (iNOS), activated by NF-KB is another
enzyme that plays a pivotal role in mediating
inflammation, especially as it acts in synergy with
COX-2.
TURMERIC - APPROVED AS FOOD ADDITIVE
Curcumin, (1,7-bis (4-hydroxy-3-methoxyphenol)1,6 heptadiene-3,5-dione), a polyphenol rich in the
dietary spice turmeric, is received from dried
rhizozomes of the perennial herb Curcuma longa
Linn, a member of the ginger family. Turmeric is
mainly known for its excellent ability to preserve
food and is approved as food additive in most
Western countries. It is produced in several Asian
and South-American countries. In India alone
about 500,000 metric tons are produced each year,
of which about half is exported. It has, in addition
to extensive use as food additive, for generations
also been used in traditional medicine for treatment
of various external or internal inflammatory
conditions such as arthritis, colitis and hepatitis.
The molecule of curcumin resembles ubiquinols
and other phenols known to possess strong
antioxidant activities. Its bioavailability on oral
supplementation is low, but can be improved by
dissolution in ambivalent solvents (glycer ol,
ethanol, DMSO) [12]. It is also reported to be
dramatically elevated by co-ingestion of peperine
(a component of pepper), demonstrated both in
experimental animals and humans [13]. Several
studies have demonstrated that curcumin is atoxic,
also in very high doses[14,15]. Treatment of humans
for three months with 8000 mg curcumin per day
showed no side effects[15]. It is estimated that adult
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KUWAIT MEDICAL JOURNAL
Indians consume 80-200 mg curcumin per day[16]. A
common therapeutic dose is 400-600 mg curcumin
three times daily corresponding to up to 60 g fresh
turmeric root or about 15 g turmeric powder. The
content of curcumin in turmeric is usually 4-5 %.
CURCUMIN- EFFECTIVE AGAINST STRESSINDUCED OVERINFLAMMATION
Curcumin is not only an inexpensive atoxic and
potent COX-2 and iNOS inhibitor[17], it is also a
potent inducer of heat shock proteins (HSPs) and
potential cytoprotector[18,19]. Curcumin does not only
inhibit COX-2, it also inhibits lipooxygenases (LOX)
and leukotreines such as LBT4 and 5HETE [20],
especially when bound to phosphatidylcholine
micelles[21]. It is also reported to inhibit cytochrome
P450 isoenzymes and thereby activation of
carcinogens[22]. Curcumin has the ability to intercept
and neutralize potent pro-oxidants and carcinogens,
both ROS (superoxide, peroxyl, hydroxyl radicals)
and NOS (nitric oxide, peroxynitrite)[23]. It is also a
potent inhibitor of TGF-β and fibrogenesis[24] which
is one of the reasons, why it can be expected to have
positive effects in diseases such as kidney fibrosis,
lung fibrosis, liver cirrhosis and Crohn’s Disease
and in prevention of formation of tissue
adhesions[25]. Curcumin is suggested to to be
especially effective in Th1-mediated immune
diseases as it effectively inhibits Th1 cytokine
profile in CD4 + T cells by interleukin-12
production[26].
Many medicinal herbs and pharmaceutical
drugs are therapeutic at one dose and toxic at
another, and interactions between herbs and drugs,
even if structurally un-related, may increase or
decrease the pharmacological and toxicological
effects of either component[27,28]. It is suggested that
curcumin may increase the bioavailability of
vitamins such as vitamin E and also decrease
cholesterol, as curcumin in experimental studies
significantly raises the concentration of αtocopherol in lung tissues and decreases plasma
cholesterol[29]. Polyphenols, isothiocyanates such as
curcumin and flavonoids such as resveratrol, are all
made accessible for absorption into the intestinal
epithelial cells and the rest of the body by
digestion/fermentation in the intestine by
microbial flora[30].
CURCUMIN IN ACUTE AND CHRONIC DISEASES
Atherosclerosis: Oxidation of low density
lipoproteins (LDL) is suggested to play a pivotal
role in the development of arteriosclerosis, and
LDL oxidation products are toxic to various types
of cells including endothelial cells. Curcumin has a
strong capacity to prevent lipid peroxidation,
stabilize cellular membranes, inhibit proliferation
269
of vascular smooth muscle cells, and inhibit platelet
aggregation; all important ingredients in the
pathogenesis of arteriosclerosis. Curcumin was
found to be the most effective and quercetin the
least, when curcumin, quercetin and capsaisin were
compared for their ability to inhibit the initiation
and propagation phases of LDL oxidation of a
defined antioxidant butylated hydroxy anisole
(BHA)[31]. Supply of curcumin, but also capsaicin
and garlic (allecin) to rats fed a cholesterol-enriched
diet prevented both increase in membrane
cholesterol and increased fragility of the
erythrocytes[32]. Significant prevention of early
atherosclerotic lesions in thoracic and abdominal
aorta are observed in rabbits fed an atherogenic diet
for thirty days, accompanied by significant
increases in plasma concentrations of coenzyme Q,
retinol and α-tocopherol and reductions in LDL
conjugated dienes and in TBARS (thiobarbituric
acid-reactive substances, an expression of ongoing
oxidation)[33].
Cancer: Cancer is a group of more than 100
different diseases, which manifest itself in
uncontrolled cellular reproduction, tissue invasion
and distant metastases[34]. Behind the development
of these diseases are, most often, exposure to
carcinogens, which produce genetic damage and
irreversible mutations, if not repaired. During the
last fifty years attempts have been made to find or
produce substances that could prevent these
processes, so called chemopreventive agents.
Cancers are generally less frequent in the
developing world, which has been associated both
with less exposure to environmental carcinogens
and to a richer supply of natural chemopreventive
agents. The incidence per 100, 000 population is in
the USA considerably higher for the following
diseases compared to India: prostatic cancer (23 X),
melanoma skin cancer (male 14 X, female 9 X),
colorectal cancer (male,11 X, female 10 X),
endometrial, cancer (9 X), lung cancer (male 7 X,
female 17 X), bladder cancer (male 7 X, female 8 X)
breast cancer (5 X), renal cancer (male 9 X, female 12
X)[35]. These differences are even greater for some
diseases such as breast cancer and prostatic cancer
when compared to China. The consumption of
saturated fat and sugary foods is much less in the
Asian countries, but equally important, the
consumption of plants with high content of
chemopreventive substances is significantly higher
in these countries. As an example, the consumption
of curcumin has for centuries been about 100
mg/day in these Asian countries [36]. Curcumin
induces in vitro apoptosis of various tumour cell
lines: breast cancer cells[36,37], lung cancer cells[38],
270
Plant-derived Health-Effects of Turmeric and Curcomenoids
human melanoma cells[39], human myeloma cells[40],
human leukemia cell lines[41], human neuroblastoma
cells[42], oral cancer cells[43], prostatic cancer cells[44-47].
Curcumin has in experimental models also
demonstrated ability to inhibit intrahepatic
metastases[48]. Few in vivo experimental studies and
no clinical controlled trials are this far concluded.
However, a recent phase I study reported histologic
improvement of precancerous lesions in one out of
two patients with recently resected bladder cancer,
two out of seven patients of oral leucoplakia, one
out of six patients of intestinal metaplasia of the
stomach, and two out of six patients with Bowen’s
disease[49]. However, the main purpose of the study
was to document that curcumin is not toxic to
humans when taken by mouth for three months in
a dose of up to 8,000 mg/day.
Diabetes: Turmeric (TU, 1 g/kg body weight) or
curcumin (CU, 0.08 g/kg body weight) were in a
recent study supplied daily for three weeks to rats
with alloxan-induced diabetes (AID) and compared
to controls (CO)[50]. Significant improvements were
observed in blood glucose (mg/dl CO 88.3, AID
204.4, TU 142.7, CU 140.1), hemoglobin (gm/dl CO
14.7, AID 10.8, TU 13.6, CU 13.1) and glycosylated
hemoglobin (gm/dl CO 2.8, AID 11.2, TU 9.0, CU
7.8). Significant differences were also observed in
TBARS in liver tissue (nmoles/g tissue CO 43.0,
AID 54.0, TU 34.0, CU 29.0), TBARS in plasma
(nmoles/ml CO 3.8, AID 7.3, TU 5.3, CU 4.6), in
glutathione in liver (µgm/mg CO 23.4, AID 11.2,
TU 16.6, CU 20.9) and glutathione in plasma
(mg/dl CO 22.4, AID 14.2, TU 18.4, CU 20.1). It was
also observed that the activity of sorbitol
dehydrogenase (SDH), which catalyzes the
conversion of sorbitol to fructose, was significantly
lowered by treatment both with turmeric and
curcumin.
Gastric diseases: When the in vitro effects against
19 different Helicobacter pylori strains, including five
cag A+ strains (cag A is the strain-specific H pylori
gene linked to premalignant and malignant lesions)
were studied, both treatments were found to be
equally effective as both treatments did significantly
reduce growth of all the strains studied[51]. Subsequent
studies did also demonstrate that curcumin inhibits
infection and inflammation of gastric mucosal cells
through the inhibition of activation of NF-KB,
degradation of IKBα, NF-KB DNA binding and the
activity of IKB kinases α and β. No curcumininduced effects were observed on mitogenactivated protein kinases (MAPK), extracellular
signal regulating kinases 1/2 (ERK1/2) and p38. H
pylori-induced mitogenic response was completely
December 2006
blocked by curcumin[52]. Significant antifungal
properties against various fungal, especially
phytopathogenic, organisms by curcumin are also
reported[53].
Hepatic diseases: Dietary supply of curcuminoids
is also reported to increase hepatic acyl-CoA and
prevent high-fat diet-induced accumulation in the
liver and adipose tissues in rats [54]. Ethanol-induced
steatosis is known to be further aggravated by
supply of PUFA-rich vegetable oils, which has been
thermally oxidized. Rats fed for 45 days with a diet
containing 20 % ethanol and 15 % sunflower oil,
heated to 180º C for 30 min (AO), showed extensive
histopathological changes with focal and feathery
degeneration, micronecroses and extensive steatosis
in the liver and extensive inflammation, vessel
congestion and fatty infiltration in the kidneys,
changes, which could largely be prevented by
simultaneous supply of curcumin (CU) or
particularly photo-irradiated curcumin (PCU) e.g.
curcumin kept in bright sunshine for five hours[55].
Both products were supplied in a dose of 80 mg/kg
body weight. Both products did significantly
inhibit elevations in alkaline phosphatases (ALP):
controls (CO) 85.88, PCU 239.56, CU 177.41 and
PCU 149.15 and _-glutamyl transferase (GGT): CO
0.60, PCU 2.51, CU 1.43, PCU 1.15. Similar
beneficial effects were observed on histology in
various tissues and in hepatic content of
cholesterol, triglycerides free fatty acids and
phospholipids. In another study, rats were fed with
fishoil and ethanol (FE) for four weeks which
resulted in hepatic lesions consisting of a fatty liver,
necrosis and inflammation. Supply of curcumin in a
daily dose of 75 mg/kg body weight to these rats
prevented the histological lesions[56]. Curcumin was
observed in part to suppress NF-KB-dependent
genes, to block endotoxin-mediated activation of
NF-KB and to suppress the expression of cytokines,
chemokines, COX-2 and iNOS in Kupffer cells.
Similar effects were also observed in carbon
tetrachloride-induced injuries. Pretreatment for
four days with curcumin (100 mg/kg body weight)
before intraperitoneal injection of CCl4 prevented
subsequent increases in TBARS significantly: CO
274, CCl4 556, CU 374, alanine aminotransferase
(ALT): CO 46, CCL4 182, CU 97 and aspertate
aminotransferase (AST): CO 97, CCl4 330, CU 211
and in hydroxyproline (µg/g liver tissue): CO 281,
CCl4 777, CU 373 [57].
Intestinal diseases: Pretreatment for ten days with
curcumin in a daily dose of 50 mg/kg body weight
before induction of trinitrobenzene sulphonic acid
(TNBS) colitis resulted in a significant reduction in
December 2006
KUWAIT MEDICAL JOURNAL
degree of histological tissue injury, neutrophil
infiltration (measured as decrease in myeloperoxidase activity) and lipid peroxidation (measured
as decrease in malondialdehyde activity) in the
inflamed colon and in a decreased serine protease
activity[58]. A significant reduction in NF- KB
activation and reduced levels of NO and a marked
suppression of Th1 functions: IFNγ and IL-12p40
mRNA, was also observed. Curcumin was in
another similarly designed study added to the diet
for five days before induction of TNBS colitis,
which resulted in a significant reduction in
myeloperoxidase, and attenuation of the TNBSinduced message for IL-1β on semiquantitative RTPCR[59]. Western blotting revealed a significant
attenuation of the activation of p38 MAPK.
Curcumin was also supplied in combination with
caffeic acid phenethyl ester (CAPE) to animals
treated with cytostatic drugs (arabinose cytosine,
Ara-C, and methotrexate, MTX)[59]. The treatment
did not only inhibit the NF-KB induced mucosal
barrier injury but was also shown to increase the in
vitro susceptibility of the non-transformed small
intestinal rat epithelial cell, IEC-6, to the cytostatic
agents.
Neurodegenerative diseases: A growing body of
evidence implicates free radical toxicity, radical
induced mutations and oxidative enzyme
impairment and mitochondrial dysfunction in
neurodegenerative diseases (NDD). Significant
oxidative damage is observed in all NDDs, which
in the case of Alzheimer disease (AD) leads to
extracellular deposition of β-amyloid (Aβ) as senile
plaques. Nonsteroidal anti-inflammatory drugs
(NSAIDs) like ibuprofen have proved effective in
preventing progress of AD in animal models[60] but
gastrointestinal and occasional liver and kidney
toxicity induced by inhibition of COX-1 precludes
widespread chronic use of the drug[61]. Use of
antioxidants such as vitamin E (α-tocopherol) has
proven rather unsuccessful even when high doses
were used[62]. Vitamin E, α-tocopherol, is in contrast
to γ-tocopherol a poor scavenger of nitric oxide(NO) based free radicals. Curcumin is several times
more potent a scavenger than vitamin E[63] and in
addition also a specific scavenger of NO-based
radicals[64]. When tried in a transgenic mouse model
of AD, a modest dose (24 mg/kg body weight), but
not a > 30 times higher dose (750 mg/kg body
weight) of curcumin significantly reduce oxidative
damage and amyloid pathology [65]. Similar
observations, reductions in both Aβ deposits and in
memory deficits are also made in Sprague Dawley
rats[66]. The age-adjusted prevalence of both AD[67]
and Parkinson’s disease (PD) is in India[68] with its
271
significantly higher intake of turmeric, much lower
than in Western countries, especially the USA.
However, the preventive effects of consumption of
turmeric can also be achieved with other
polyphenol-rich fruits and vegetables if consumed
in enough quantities. Blueberries, strawberries and
spinach in doses of 18.6, 14.8 and 9.1 gm of dried
extract/kg body weight were demonstrated to be
effective in reversing age-related deficits in both
neuronal and behavioural parameters[69]. A study
from 1999 is of special interest: Rats on chronic
ethanol supply were randomized to 80 mg/kg
body weight of curcumin (CU) or control (CO) and
compared to non-intoxicated normal rats (NI)[70].
The degree of histopathological changes, the levels
of TBARS (NI 1.29, CU 2.41, CO 2.98), cholesterol
(NI 1531.9, CU 1658.2, CO 2031.1), phospholipids
(NI 1845.5, CU 2011.5, CO 2795.1), and free fatty
acids (NI 26.7, CU 39.9, CO 53.1) in brain tissue
were significantly improved after curcumin
treatment.
Ocular diseases: Cataract, an opacity of the eye
lens, is the leading cause of blindness worldwide,
responsible for the blindness of almost 20 million
people in the world[71]. Nutritional deficiencies,
especially lack of consumption of enough
antioxidants, diabetes, excessive sunlight, smoking
and other environmental factors are known to
increase the risk of cataracts[72]. The age-adjusted
prevalence of cataract in India is, however, three
times that of the United States [73]. Despite this, three
different experimental studies have reported
significant preventive effects of curcumin against
cataracts induced by naphthalene[74], galactose[75]
and selenium[76].
Pancreatic diseases: The effect of curcumin to
reduce the damage to pancreas was studied in two
different models; cerulein-induced and ethanol and
CCK-induced pancr eatitis[77]. Curcumin was
administered intravenously in parallel with
induction of pancreatitis. A total of 200 mg/kg
body weight was administered during the
treatment period of six hours. Curcumin treatment
significantly reduced histological injuries, the
acinar cell vacuolization and neutrophil infiltration
of the pancreatic tissue, the intrapancreatic
activation of trypsin, the hyperamylasemia and
hyperlipasemia, and the pancreatic activation of
NF-KB, IKB degradation, activation of activator
protein (AP)-1and various inflammatory molecules
such as IL-6, TNF-α, chemokine KC, iNOS and
acidic ribosomal phosphoprotein (ARP). Curcumin
did also significantly stimulate pancreatic
activation of caspase-3 in both models.
272
Plant-derived Health-Effects of Turmeric and Curcomenoids
Respiratory diseases: As mentioned above,
curcumin is a potent inhibitor of TGF-β and
fibrogenesis[25] and is thought to have positive
effects in fibrotic diseases in kidneys, liver, intestine
(Crohn’s Disease), body cavities (prevention of
fibrous adhesions)[19] and on conditions with lung
fibrosis, including cystic fibrosis. The latter is of
special interest as it has been especially linked to
glutathione deficiency. The effect of curcumin
against amiodarone-induced lung fibrosis was
recently studied in rats[78]. Significant inhibition of
LDH activity, infiltration of neutrophils, eosinophils
and macrophages in lung tissue, LPS-stimulated
TNF-α release, phorbole myristate acetate (PMA)stimulated superoxide generation, myeloperoxidase
(MPO) activity, TGF- β1 activity, lung hydroxyproline
content and expression of type I collagen and c-Jun
protein were observed when curcumin was
supplemented in doses of 200 mg/kg body weight
in parallel with intratracheal instillation of 6.25
mg/kg body weight of amiodarone. Curcumin
exhibits structural similarities to isoflavonoid
compounds that seem to bind directly to the CFTR
protein and alter its channel properties[79]. Egan et
al[80], who had previously observed that curcumin
inhibits a calcium pump in endoplasmic reticulum,
thought that reducing the calcium levels might
liberate the mutant CFTR and increase its odds of
reaching the cell surface (see also)[81]. The ∆F508
mutation, the most common cause of cystic fibrosis,
will induce a misprocess in the endoplasmatic
reticulum of a mutant cystic fibrosis transmembrane
conductance regulator (CFTR) gene. A dramatic
increase in survival rate and in normal cAMPmediated chloride transport across nasal and
gastrointestinal epithelia was observed in genetargeted mice homozygous for the ∆F508 when
supplemented curcumin[79]. No human studies are
yet reported and it is too early to know if this
treatment will be able to halt or reverse the decline
in lung function also in patients with cystic fibrosis.
An eventual anti-asthmatic effect of curcumin was
recently tested in guinea-pigs sensitized with
ovalbumin and significant reductions observed
both in airway constriction and in airway
hyperreactivity to histamine[82].
Tobacco/cigarette smoke (CS)-induced injuries:
CS is suggested to cause 20% of all deaths and
~30% of all deaths from cancer. CS contains
thousands of compounds of which about hundred
are known carcinogens, co-carcinogens, mutagens
and/or tumor promoters. Each puff of smoke
contains over 10 trillion free radicals. Antioxidant
levels in blood are also significantly reduced in
smokers. Activation of NF-KB has been implicated
in chemical carcinogenesis and tumorigenesis
December 2006
through activation of several genes such as COX-2,
iNOS, matrix metalloproteinase ((MMP)-9, IL-8,
cell surface adhesion molecules anti-apoptotic
protein and others. A recent study reports that
curcumin abrogates the activation of NF-KB, which
correlates with down-regulation of COX-2, MMP-9
and cyclin D1 in human lung epithelial cells[83].
PLANT ANTIOXIDANTS - RELEASED BY GI
MICROBES (Flora)
All chronic diseases are in a way related. They
all develop as a result of a prolonged and
exaggerated inflammation [84]. Their development
can most likely be prevented or at least delayed by
extensive consumption of antioxidants such as
curcumin. It is important to remember, that it is
almost exclusively through microbial fermentation
of the different plants that bioactive antioxidants
are released and absorbed. Clearly flora and
supplied lactic acid bacteria/probiotics play an
important role. It is therefore unfortunate that both
size and diversity of flora is impaired and intake of
probiotic bacteria significantly reduced among
Westerners. For example, reduction in total
numbers and diversity of flora is also associated
with certain chronic diseases such as IBD[85].A study
from 1983 demonstrated that Lb plantarum, a strong
fibre fermentor, is found in only 25% of omnivorous
Americans and in about
2/3 of vegetarian
Americans[86]. Great differences in volume and
diversity of flora have also been observed between
different human cultures. It is reported that
Scandinavian children as compared to Pakistani
children have a much reduced flora[87]. Astronauts,
who return from space flights have during the
flight lost most of their commensal flora including
lactobacillus species such as Lb plantarum (lost to
almost 100%), Lb casei (lost to almost 100%), Lb
fermentum (reduced by 43%), Lb acidophilus
(reduced by 27%), Lb salivarius (reduced by 22%)
and Lb brevis (reduced by 12%)[88], changes most
likely attributed to poor eating (dried food, no fresh
fruits and vegetables) and a much reduced intake of
plant fibers and natural antioxidants, to the mental
and physical stress and eventually also to the lack
of physical exercise. Many individuals in Western
Societies exhibit a type of “astronaut-like lifestyle”
with unsatisfactory consumption of fresh fruits,
vegetables, too much stress and no or little
outdoor/sport activities. Furthermore, flora seems
not to tolerate exposure to chemicals including
pharmaceuticals. This is also demonstrated in
critically ill, who most often have lost their entire
lactobacillus flora[89]. A recent Scandinavian study
suggest that fiber-fermenting LAB such as Lb
plantarum, Lb rhamnosus and Lb paracasei ssp
paracasei, present in all humans with a rural
December 2006
KUWAIT MEDICAL JOURNAL
lifestyle, are only found 52%, 26% and 17%
respectively of persons with a more urban Western
type lifestyle[90]. These LAB are present in all with
more rural lifestyle. The lack of these LAB is
probably negative as these LAB are unique in their
ability to ferment important fibers such as inulin
and phlein, otherwise resistant to fermentation by
most lactobacillus species[91], and superior to other
lactobacillus in their ability to eliminate pathogenic
microorganisms such as Clostridium difficile[92].
CONCLUSIVE REMARKS
To use medicinal plants and their active
components is becoming an increasingly attractive
approach for the treatment of various inflammatory
disorders among patients unresponsive or unwilling
to take standard medicines. Food derivates have
the advantage of being relatively nontoxic. This is
certainly so for turmeric and curcumin. If one
chooses to supply it with the fiber, e.g., as turmeric,
additional supplementation with probiotic bacteria
will most likely enhance the efficacy of treatment.
Increasing evidence suggest that as saturated fat
in the diet increases and plant fibre intake reduces
the inflammatory reaction in the body increases[93].
A high fat/low fibre diet is clearly associated with
chronic diseases[94] and fruit and vegetable intake
with reduction in incidence of chronic diseases[95].
Focus is increasingly turning from fibre per se to
active ingredients in the plant fibres, antioxidants
and anti-inflammatory agents such as curcuminoids
in turmeric.
Not only turmeric and curcumin, but also
numerous other plants contain compounds which
reduces inflammation and protect against disease.
Among them are several thousands of plantderived chemo-preventive agents, polyphenols and
many other, most often unexplored, substances,
which seem to have potential to reduce inflammation,
speed of aging, and prevent degenerative malfunctions
of organs and development of chronic diseases.
Among them isothiocyanates in cruciferous
vegetables, anthocyanins and hydroxycinnamic
acids in cherries, epigallocatechin-3-gallate (EGCG)
in green tea, chlorogenic acid and caffeic acid in
coffee beans and also in virgin tobacco leaves,
capsaicin in hot chili peppers, chalcones in apples,
euginol in cloves, gallic acid in rhubarb, hisperitin
in citrus fruits, naringenin in citrus fruits,
kaempferol in white cabbage, myricetin in berries,
rutin and quercetin in apples and onions,
resveratrol and other procyanidin dimers in red
wine and virgin peanuts, various curcumenoids,
the main yellow pigments in turmeric curry foods,
and daidzein and genistein from the soy bean.
These compounds have all slightly different
functions and seem to complement each other well.
273
REFERENCES
1.
2.
3.
4.
5.
6.
7.
8.
9.
10.
11.
12.
13.
14.
15.
16.
17.
18.
19.
20.
21.
World Health Organisation. Process for a global strategy on
diet, physical activity and health. WHO Geneva February
2003.
Arias E, Smith BL. Deaths: preliminary data for 2001. Natl
Vital Stat Rep 2003; 51:1-44.
Angus DC, Linde-Zwirble WT, Lidicker J, Clermont G,
Carcillo J, Pinsky MR. Epidemiology of severe sepsis in the
United States:analysis of incidence, outcome and associated
costs of care. Crit Care Med 2001; 29:1303-1310.
Baptista JAB, Carvalho RCB. Indirect determination of
Amadori compounds in milk-based products by
HPLC/ELSD/UV as an index of protein detorioration.
Food Research International 2004; 37:739-747.
Bengmark S. Acute and “chronic” phase response - a
mother of disease. Clin Nutr 2004; 23:1256-1266.
Bengmark S. Bio-ecological Control of the Gastrointestinal
Tract: The Role of Flora and Supplemented Pro- and
Synbiotics. Gastroenterol Clin North Am 2005; 34:413-436.
Bengmark S. Impact of nutrition on ageing and disease.
Curr Opin Nutr Metab Care 2006; 9:2-7.
Bernes PJ, Karin M. Nuclear factor-kappaB: a pivotal
transcription factor in chronic inflammatory diseases. N
Engl J Med 1997; 336:1066-1071.
Amit S, Ben-Neriah Y. NF-kappaB activation in cancer: a
challenge for ubiquitination- and proteasome-based
therapeutic approach. Semin Cancer Biol 2003; 13:15-28.
Pahl HL. Activators vand target genes of Rel/ NF- KB
transcription factors. Oncogene 1999; 18:6853-6866.
Stolina M, Sharma S, Lin Y, et al. Specific inhibition of
cyclooxygenase-2 restores antitumor reactivity by altering
the balance of IL-10 and IL-12 synthesis. J Immunol 2000;
164:361-370.
Sharma RA, Ireson CR, Verschoyle RD, et al. Effects of
dietary curcumin on glutathione S-transferase and
malonaldehyde-DNA adducts in rat liver and colonic
mucosa: relationship with drug levels. Clin Cancer Res.
2001; 7:1452-1458.
Shoba G, Joy D, Joseph T, et al. Influence of peperine on the
pharmacokinetics of curcumin in animals and human
volunteers. Planta Med 1998; 64:1167-1172.
Bhavani Shankar TN, Shantha NV, Ramesh HP, et al.
Toxicity studies on Turmeric (Curcuma longa): acute
toxicity studies in rats, guinea pigs & monkeys. Indian J
Exp Biol 1980; 18:73-75.
Chainani.Wu N. Safety and anti-inflammatory activity of
curcumin: a component of turmeric (Curcuma Longa). J
Alternative and Complementary Medicine 2003; 9:161-168.
Grant KL, Schneider CD. Turmeric. Am J Health-Syst
Pharm 2000; 57:1121-1122.
Surh Y-J, Chun K-S, Cha H-H, et al. Molecular mechanisms
underlying chemo-preventive activities of antiinflammatory phytochemicals: downregulation of COX-2
and iNOS through suppression of NF- KB activation.
Mutation Research 2001; 480-481:243-268.
Dunsmore KE, Chen PG, Wong HR. Curcumin, a medicinal
herbal compound capable of inducing the heat shock
response. Crit Care Med 2001; 29:2199-2204.
Chang D-M. Curcumin: a heat shock response inducer and
potential cytoprotector. Crit Care Med 2001; 29;2231-2232.
Wallace JM Nutritional and botanical modulation of the
inflammatory cascade - eicosanoids, cyclooxygenases and
lipooxygenases - as an adjunct in cancer therapy.
Integrative Cancer Therapies 2002; 1:7-37.
Began G, Sudharshan E, Udaya Sankar K, et al. Interaction
of curcumin with phosphatidylcholine: a spectrofluorometric
study. J Agric Food Chem 1999; 47:4992-4997.
274
Plant-derived Health-Effects of Turmeric and Curcomenoids
22. Thapliyal R, Maru GB. Inhibition of cytochrome P450
isoenzymes by curcumins in vitro and in vivo. Food and
Chemical Toxicology 2001; 39:541-547.
23. Jovanovic SV, Boone CW, Steenken S, et al. How curcumin
preferentially works with water soluble antioxidants. J Am
Chem Soc 2001; 23:3064-3068.
24. Gaedeke J, Noble NA, Border WA. Curcumin blocks
multiple sites of the TGF-β signaling cascade in renal cells.
Kidney International 2004; 66:112-120.
25. Srinisan P, Libbus B. Mining MEDLINE for implicit links
between dietary substances and diseases. Bioinformatics
2004; 20:1290-1296.
26. Kang BY, Song YJ, Kim KM, et al. Curcumin inhibits Th1
cytokine profile in CD4+ T cells by suppressing interleukin12 production in macrophages. Br J Pharmacol 1999;
128:380-384.
27. Fugh-Berman A. Herb-drug interactions. Lancet 2000;
355:134-138.
28. Groten JP, Butler W, Feron VJ, et al. An analysis of the
possibility for health implications of joint actions and
interactions between food additives. Reg. Toxicol
Pharmacol 2000; 31:77-91.
29. Kamal-Eldin A, Frank J, Razdan A, et al. Effects of dietary
phenolic compounds on tocopherol, cholesterol and fatty
acids in rats. Lipids 2000; 35:427-435.
30. Shapiro TA, Fahey JW, Wade KL, et al. Human metabolism
and excretion of cancer chemoprotective glucoisonolates
and isothiocyanates of cruciferious vegetables. Cancer
Epidemiol Biomarkers Prev 1998; 7:1091-1100.
31. Akhilender Naidu K, Thippeswamy NB. Inhibition of
human low density lipoprotein oxidation by active
principles from spices. Mol Cell Biochem 2002; 229:19-23.
32. Kempaiah RK, Srinivasan K. Integrity of erythrocytes of
hypercholesterolemic rats during spices treatment. Mol Cell
Biochem 2002; 236:155-161.
33. Quiles JL, Dolores Mesa M, César L, et al . Curcuma longa
extraxt supplementation reduces oxidative stress and
attenuates aortic fatty streak development in rabbits.
Arterioscler Throm Vasc Biol 2002; 22:1225-1231.
34. Levi MS, Borne RF, Williamson JS. A review of cancer
chemopreventive agents. Current Medicinal Chemistry
2001; 8:1349-1362.
35. Anderson SR, McDonald SS, Greenwald P. J Postgrad Med
2003; 49:222-228.
36. Choudhuri T, Pal S, Munna L, et al. Curcumin induces
apoptosis in human breast cancer cells through p53dependent Bax induction. FEBS Letters 2002; 512:334-340.
37. Shao ZM, Shen ZZ, Liu CH, et al. Curcumin exerts multiple
suppressive effects on human breast cardinoma cells. Int J
Cancer 2002; 98:2002.
38. Pillai GR, Srivastava AS, Hassanein TI, et al. Induction of
apoptosis in human lung cancer cells by curcumin. Cancer
Letters 2004; 208:163-170.
39. Zheng M, Ekmekcioglu S, Walch ET, et al. Inhibition of
nuclear factor- KB and nitric oxide by curcumin induces
G2/M cell cycle arrest and apoptosis in human melanoma
cells. Melanoma Res 2004; 14:165-171.
40. Han SS, Keum YS, Seo HJ, Surh YJ. Curcumin suppresses
activation of NF-KB and AP-1 induced by phorbol ester in
cutured human promyelocytic leukaemia cells. J Biochem
Molecul Biol 2002; 35:337-242.
41. Bharti AC, Shishodia S, Reuben JM, et al. Nuclear factor- _B
and STAT3 are constitutively active in CD138+ cells derived
from myeloma patients and suppression of these
transcription factors leads to apoptosis. Blood 2004;
103:3175-3184.
42. Liontas A, Yeger H. Curcumin and resveratrol induce
apoptosis and nuclear translocation and activation of p53 in
December 2006
human neuroblastoma. Anticancer Res 2004; 24:987-998.
43. Elattar TMA, Virji AS. The inhibitory effect od curcumin.
Genistein, quercetin and cisplatin on the growth of oral
cancer cells in vitro. Anticancer Res 2000; 20:1733-1738.
44. Mukhopadhyay A, Bueso-Ramos C, Chatterjee D, et al.
Curcumin downregulates cell survival mechanisms in
human prostate cancer cell lines. Oncogene 2001; 20:75977609.
45. Nakamura K, Yasunaga Y, Segawa T, et al. Curcumin downregulates AR gene expression in prostate cancer cell lines.
Int J Oncol 2002; 21:825-830.
46. Hour TC, Chen J, Huang CY, et al. Curcumin enhances
cytotoxicity of chemotherapeutic agents in prostate cancer
cells by inducing p21WAFI/CIPI and C/EBPβ expressions and
suppressing NF-KB activation. The Prostate 2002; 51:211218.
47. Deab D, Jiang H, Gao X, et al. Curcumin sensitizes prostate
cancer cells to tumor necrosis factor-related apoptosisinducing ligand/Apo2L by inhibiting nuclear factor- KB
through suppression of I KBα phosphorylation. Mol Cancer
Ther 2004; 3:803-812.
48. Ohadshi Y, Tsuchia Y, Koizumi K, et al. Prevention of
intrahepatic metastasis by curcumin in an orthotopic
implantation model. Oncology 2003; 65:250-258.
49. Cheng AL, Hsu CH, Lin JK, et al. Phase I clinical trial of
curcumin, a chemopreventive agent, in patients with highrisk or pre-malignant lesions. Anticancer Res. 2001; 21:28952900.
50. Giltay EJ, Hoogeveen EK, Elbers JMH, et al. Insulin
resistance is associated with elevated plasma total
homocysteine levels in healthy, non-obese subjects. Letter
to the Editor. Atherosclerosis 1998; 139:197-198.
51. Mahady GB, Pendland SL, Yun G, Lu ZZ. Turmeric
(Curcuma longa) and curcumin inhibit the growth of
Helicobacter pylori, a group 1 carcinogen. Anticancer
Research 2002; 22:4179-4182.
52. Foryst-Ludwig A, Neumann M, Schneider-Brachert W,
Naumann M. Curcumin blocks NF-KB and the mitogenic
response in Helicobacter pylori-infected epithelial cells.
Biochem Biophys Res Com 2004; 316:1065-1072.
53. Kim MK, Choi GJ, Lee HS. Fungal property of Curcuma
longa rhizome-derived curcumin against phytopathogenic
fungi in greenhouse. J Agr Food Chem 2003; 51:1578-1581.
54. Asai A, Miyazawa T. Dietary corcuminoids prevent high-fat
diet-induced lipid accumulation in rat liver and epididymal
adipose tissue. J Nutr 2001; 131:2932-2935.
55. Rukkumani R, Balasubashini S, Vishwanathan P, Menon
VP. Comparative effects of curcumin and photo-irradiated
curcumin on alcohol- and polyunsaturated fatty acidinduced hyperlipidemia. Pharmacol Res 2002; 46:257-264.
56. Nanji AA, Jokelainen K, Tipoe GL, et al. Curcumin prevents
alcohol-induced liver disease in rats by inhibiting the
expression of NF- KB-dependent genes. Am J Physiol
Gastrointest Liver Physiol 2003; 284:G321-G327.
57. Park EJ, Jeon CH, Ko G, et al. Protective effect of curcumin
in rat liver injury induced by carbon tetrachloride. J Pharm
Pharmacol 2000; 52:437-440.
58. Ukil A, Maity S, Karmakar S, et al. Curcumin, the major
component of food flavour turmeric reduces mucosal injury
in trinitrobenzene sulphonic acid-induced colitis. Br J
Pharmacol 2003; 139:209-218.
59. van’t Land B, Blijlevens NMA, Marteijn J, et al. Role of
curcumin and the inhibition of NF- KB in the onset of
chemotherapy-induced mucosal barrier injury. Leukemia
2004; 18:276-284.
60. Lim GP, Yang F, Chu T, et al. Ibufprofen suppresses plaque
pathology and inflammation in a mouse model for
Alzheimer’s disease. J Neurosci 2000; 20:5709-5714.
December 2006
KUWAIT MEDICAL JOURNAL
61. Bjorkman D. Nonsteroidal anti-inflammatory drugassociated toxicity of liver, lower gastrointestinal tract, and
esophagus. Am J Med 1998; 105:S17-S21.
62. Sano M, Ernesto C, Thomas RG, et al.A controlled trial of of
selegiline, alpha-tocopherol, or both as treatment for
Alzheimer disease. The Alzheimer disease cooperative
study. N Engl J Med 1997; 336:1216-1222.
63. Zhao BL, Li XJ, He RG, et al. Scavenger effects of green tea
and natural antioxidants on active oxygen radicals. Cell
Biophys 1989; 14:175-185.
64. Sreejavan N, Rao MNA. Nitric oxide scavenging by
curcumenoids. J Pharm Pharmacol 1997; 49:105-107.
65. Lim GP, Chu T, Yang F, et al. The curry spice curcumin
reduces oxidative damage and amyloid pathology in an
Alzheimer trangenic mouse. J Neurosci 2001; 21:8370-8377.
66. Frautschy SA, Hu W, Kim P, et al. Phenolic antiinflammatory antioxidant reversal of Aβ-induced cognitive
deficits and neuropathology. Neurobiol Aging 2001; 22:9931005.
67. Ganguli M, Chandra V, Kamboh MI, et al. Apolipoprotein E
polymorphism and Alzheimer disease : the Ino-US crossnational dementia study. Arch Neurol 2000; 57:824-830.
68. Muthane U, Yasha TC, Shankar SK. Low numbers and no
loss of melanized nigral neurons with increasing age in
normal human brains from India. Ann Neurol 1998; 43:283287.
69. Joseph JA, Shukitt-Hale B, Denisova NA, et al. Reversal of
age-related declines in neuronal signal transduction,
cognitive and motor behavioural defecits with blueberry,
spinach and strawberry dietary supplementation. J
Neurosci 1999; 19:8114-78121.
70. Rajakrishnan V, Viswanathan P, Rajasekharan N, Menon
VP. Neuroprotective role of curcumin from Curcuma longa
on ethanol-induced brain damage. Phytother Res 1999;
13:571-574.
71. Thylefors B. Prevention of blindness - WHO’s mission for
vision. World Health Forum 1998; 19:53-59.
72. Ughade SN, Zodpey SP, Khanolkar VA. Risk factors for
cataract: a case control study. Indian J Ophtalmol 1998;
46:221-227.
73. Brian G, Taylor H. Cataract blindness - challenges for the
21st century. Bull World Health Organ 2001; 79:249-256.
74. Pandya U, Saini MK, Jin GF, et al. Dietary curcumin
prevents ocular toxicity of naphthalene in rats. Toxicology
letters 2000; 115:195-204.
75. Suryanarayana P, Krishnaswamy K, Reddy B. Effects on
galactose-induced cataractogenesis in rats. Molecular
Vision 2003; 9:223-230.
76. Padmaja S, Raju TN. Antioxidant effects in selenium
induced cataract of Wistar rats. Ind J Exp Biol 2004; 42:601603.
77. Gukocvsky I, Reyes CN, Vaquero EC, et al. Curcumin
ameliorates ethanol and nonethanol experimental pancreatitis.
Am J Physiol Gastrointest Liver Physiol 2003; 284:G85-G95.
78. Punithavatihi DP, Venkatesan N, Babu M. Protective effects
of curcumin against amimodarone-induced pulmonary
275
fibrosis in rats. Br J Pharmacol 2003; 139:1342-1350.
79. Illek B, Lizarzaburu ME, Lee V, Nantz MH, Kurth MJ,
Fischer H. Structural determinants for activation and block
of CFTR-mediated chloride currents by apigenin. Am J
Physiol Cell Physiol 2000; 279:C1838-C1844.
80. Egan ME, Pearson M, Weiner SA, et al. Curcumin, a major
constituent of turmeric, corrects cystic fibrosis defects.
Science 2004; 304:600-602.
81. Zeitlin P. Can curcumin cure cystic fibrosis? N Engl J Med
2004; 351:606-608.
82. Ram A, Das M, Ghosh B. Curcumin attenuates allergeninduced hyperresponsiveness in sensitized guinea pigs.
Biol Pharm Bull 2003; 26:1021-1024.
83. Shishodia S, Potdar P, Gairola CG, Aggarwal BB. Curcumin
(diferuloylmethane) down-regulates cigarette smokeinduced NF- KB activation through inhibition of IKBα kinase
in human lung cancer epithelial cells: correlation with
suppression of COX-2, MM-9, cyclin D1. Carcinogenesis
2003; 7:1269-1279.
84. Bengmark S. Acute and “chronic” phase response - a
mother of disease. Clin Nutr. 2004; 23:1256-1266.
85. Ott SJ, Wenderoth DF, Hampe J, et al. Reduction in diversity
of the colonic mucosa associated bacterial microflora in
patients with active inflammatory bowel disease. Gut 2004;
53:685-693.
86. Finegold SM, Sutter VL, Mathisen GE. Normal indigenous
intestinal flora. In: Hentges DJ, editor. Human intestinal
microflora in health and disease. London; Academic Press,
1983, p 3-31.
87. Adlerberth I, Carlsson B, deMan P, et al. Intestinal
colonization with Enterobacteriaceae in Pakistani and
Swedish hospital-delivered infants. Acta Pediatr Scandinav
1991; 80:602-610.
88. Lencner AA, Lencner CP, Mikelsaar ME, et al. Die
quantitative Zusammensetzung der Lactoflora des
Verdauungstrakts vor und nach kosmischen Flügen
unterschiedlicher Dauer Die Nahrung 1984; 28:607-613.
89. Knight DJW, Ala’Aldeen D, Bengmark S, Girling KJ. The
effect of synbiotics on gastrointestinal flora in the critically
ill. Abstract. Br J Anaesth 2004; 92:307P-308P.
90. Ahrné S, Nobaek S, Jeppsson B, et al. The normal
lactobacillus flora in healthy human rectal and oral mucosa.
J Appl Microbiol 1998; 85:88-94.
91. Müller M, Lier D. Fermentation of fructans by epiphytic
lactic acid bacteria. J Appl Bact 1994; 76:406-411.
92. Naaber P Smidt I, Stsepetova J, et al. Inhibition of
Clostridium difficile strains by intestinal Lactobacillus species.
Med Microbiol 2004; 53:551-554.
93. King DE, Egan BM, Geesey ME. Relation of dietary fat and
fiber to elevation of C-reactive protein. Am J Cardiol 2003;
92:1335-1339.
94. Campbell TC, Junchi C. Diet and chronic degenerative
diseases: perspective from China. Am J Clin Nutr 1994;
59:S1153-S1163.
95. Knekt P, Kumpulainen J, Järvinen R, et al. Flavonoid intake
and risk of chronic diseases. Am J Clin Nutr 2002; 76:560568.
KUWAIT MEDICAL JOURNAL
December 2006
Original Article
Feasiblity and Clinical Significance of Echocardiographic
Assessment of Aortic Root Compliance in Hypertensive
Patients
Aly Mohamad Hegazy, Laila Soud M Al-Einzi, Mohamad Hussain Al-Kandary, Bader Abdelkader
Department of Medicine, Non-Invasive Cardiac Laboratory, Farwania Hospital, Kuwait
Kuwait Medical Journal 2006, 38 (4): 276-283
ABSTRACT
Objectives: To evaluate the hypothesis that hypertension
is associated with reduced aortic compliance and the stiff
aortic root is a marker for prediction of associated
coronary artery disease (CAD).
Design: Cohort study conducted between January 2003
and July 2005.
Setting: Non-invasive cardiac laboratory, Department of
Medicine, Farwania Hospital, Kuwait.
Patients and Methods: One hundred and forty hypertensive
patients and 30 normotensive subjects were included in
the study. All patients underwent a 24-hour ambulatory
blood pressure recording, hand-grip isometric exercise
echocardiography and treadmill exercise ECG test. Only
100 hypertensive patients were known to have undergone
coronary angiography in the course of their clinical
management and were classified into two subgroups;
group Ia: included 60 patients with CAD and group Ib:
included 40 patients with normal coronary angiography.
Results: There was a significant increase in aortic root
area (p < 0.05) in the normotensives after isomeric
exercise but no significant change (p = NS) in the
hypertensive patients. There was a significant reduction
in aortic root compliance (p < 0.05) in the hypertensive
patients than the subjects with normal blood pressure
and in the hypertenisve patients with CAD than the
hypertensive patients with normal coronary angiography
(p < 0.05). There was a significant correlation between the
blood pressure load as an independent variable and the
aortic root compliance as a dependent variable (r = 0.873,
p < 0.05). Predictive indices revealed that reduced aortic
root compliance is valid as an indicator for the prediction
of CAD as compared to ischemic heart disease (sensitivity
= 69% Vs 60%, specificity = 71% Vs 67%, accuracy = 70%
Vs 60.7%, positive predictive value = 81.8% Vs 46.2% and
negative predictive value = 55.5% Vs 73.3%, respectively).
Stepwise multivariate analysis revealed a significant
relationship between age, gender, smoking status and
hypercholesterolemia and reduced aortic root compliance
in hypertensive patients (p < 0.05).
Conclusion: Aortic root compliance is compromised in
the hypertensive patients when compared with
normotensives subjects and its detection is of clinical
significance as the stiff aortic root can be considered a
marker for prediction of the associated CAD.
KEY WORDS: aortic root, isometric exercise, transthoracic echocardiography
INTRODUCTION
Aorta functions not only as a conduit delivering
blood to the tissues but as an important modulator
of the entire cardiovascular system, buffering the
intermittent pulsatile output from the heart to
provide steady flow to capillary beds[1]. By virtue of
its elastic properties aorta influences left
ventricular function and coronary blood flow[2].
Systemic hypertension, a common disorder with
potentially serious complications, exerts further ill
effects through structural and functional
modifications of the arterial wall[3]. Previous studies
using different techniques have shown that aortic
elastic properties are compromised in patients with
arterial hypertension [4]. Roy [5] reported that
athersclerotic plaques were present diffusely in
coronary artery disease of all adult necropsied
patients whether with or without symptomatic
ischemic heart disease and similar complicated
atherosclerotic plaques were present in the aorta as
well. Stefanadis et al from University of Athens,
Greece described a method of obtaining aortic
pressure-diameter relationship in conscious humans.
With this method, aortic diameters were acquired
with a high-fidelity intravascular catheter developed
in our institution that has an ultrasonic displacement
meter at its distal end. Aortic pre s s u res were
acquired simultaneously and at the same aortic
level with a catheter-tip micro m a n o m e t e r [6].
Measurement of pulse wave velocity has been
extensively used providing only indirect estimations
of the elastic properties of the aorta[7].
Address correspondence to:
Dr. Aly M. Hegazy, MB,BCh, MSc, MD, Department of Medicine, Non-Invasive Cardiac Laboratory, Farwania Hospital, Kuwait. Tel: (0) (965)
488-2379, E-Mail: [email protected]
December 2006
KUWAIT MEDICAL JOURNAL
The aims of the study were to:
1. Evaluate the aortic root compliance in
hypertensive patients by echocardiogram.
2. Study the association of CAD and reduced
aortic root compliance.
3. Investigate the validity and reliability of
aortic root compliance to predict the
associated CAD.
PATIENTS AND METHODS
Study patients:
One hundred and forty hypertensive patients
and 30 control subjects were included in the study.
All patients were referred by their physicians to the
cardiology clinic at Farwania Hospital with a blood
pressure more than 140/90 mmHg. All patients
were evaluated clinically by looking at history,
physical examination, 12-leads ECG and routine
laboratory investigations.
Exclusion criteria included patients with history
of myocardial infarction, unstable angina, left main
CAD, three vessel disease, intraventricular conduction
disturbances, strain patterns due to left ventricular
hypertrophy, atrial fibrillation, frequent ventricular
ectopics, retinopathy, nephropathy, diabetes mellitus,
cerebrovascular disease, significant valvular disease
and pregnant women.
Exclusion was based on: medical history,
physical examination, fundus examination, urine
analysis for proteinuria and 12-lead electrocardiogram to avoid confounding factors.
There were two groups:
Group I: included 140 hypertensive patients
(120 males and 20 females)
Group II: included 30 normotensive control
subjects (25 males and 5 females)
Coronary angiography:
Only 100 hypertensive patients were known to
have undergone coronary angiography in the
course of their clinical management and were
classified into two subgroups:
1. Group Ia: included 60 hypertensive patients
with angiographically documented coronary
artery disease.
2. Group Ib: included 40 hypertensive patients
with normal coronary angiography.
Blood pressure measurements:
Mercury sphygmomanometer was used to
measure office systolic and diastolic BP (mmHg).
At least two measurements were recorded between
8 and 11 am with the patients in a sitting position
with the legs uncrossed and the feet on the floor.
Patients were requested to refrain from heavy
exercise in the morning and to avoid cola drink,
277
coffee, tea and smoking for at least one hour before
the measurement. BP was measured after the
patients had rested for 15 minutes. The last five
minutes of rest were spent in the measurement
room with the cuff around the right upper arm.
Cuff inflation pressure was then determined by
palpating the disappearance and appearance of the
radial pulse.
Ambulatory blood pressure was recorded with
an auscultatory device (Accutracker II). Correct
position of the microphone was identified by
palpating the brachial artery. Ambulatory BP was
recorded during daytime (6 am to 10 pm) at onehour intervals and during the night (10 pm to 6 am)
at 2-hour intervals. Sleep time was identified by the
patient’s diary.
Blood pressure load is the percentage of all
systolic and diastolic BP recordings exceeding the
threshold of 140/90 mmHg[8]. Pulse pressure was
calculated as the difference between systolic and
diastolic blood pressure. Mean blood pressure was
calculated as diastolic blood pressure plus one third
pulse pressure[8].
Treadmill exercise ECG test protocol:
All patients in the study underwent the exercise
ECG test using standard or modified Bruce models.
Resting blood pressure (measured manually by
arm-cuff sphygmomanometer) was measured in
supine and standing positions before the test.
Patients with orthostatic hypotension (defined as a
decrease of > 20 mmHg of systolic blood pressure
after standing) were excluded. Resting ECG was
done for all patients to exclude patients with
significant ST- segment changes, left bundle branch
block or tachyarrhythmias. Blood pressure was
recorded midway through each stage and at peak
exercise.
The stress ECG test was terminated if there was
a decrease in blood pressure (> 20 mmHg),
significant arrhythmias (non-sustained or sustained
ventricular tachycardia), typical chest pain (test
limiting angina) or > 2 mm ST-segment depression
from baseline was noted[9]. Peak heart rate (HR):
achieved percentage of age - related peak heart rate
= (peak HR/220 - age) x 100.
Design of the study:
All patients and normotensive control subjects
were informed about the study protocol. They
underwent identical study protocol, transthoracic
echocardiography and blood pressure measurement
at rest and after hand-grip isometric exercise.
Assessment of aortic root compliance:
In order to assess aortic root compliance (C),
aortic root area (A) was calculated from each
measured aortic root dimension (D), assuming the
278
Feasiblity and Clinical Significance of Echocardiographic Assessment of Aortic Root ....
aorta to be a cylinder with formula: A = π D2/4.
Aortic root area (A) was normalized for body
surface area in order to account for individual
variability related to body size.
Aortic root compliance (C) can be defined by
C=∆A/∆P (cm2/m2/mmHg). Where ∆A is the
variation of aortic root area index between
measurements at rest and during isometric exercise
and ∆P is the variation of pressure between
measurements at rest and after isometric exercise[10].
Echocardiographic study:
Two-dimensional and M-mode echocardiography
was performed for all patients in the study using
Toshiba Power Vision and a 3.5 MHZ phased array
transducer. Measurements were performed according
to the recommendations of the American Society of
Cardiology[11]. The leading edge to leading edge
convention was used. Left ventricular dimensions
were measured at or immediately below the tips of
mitral leaflets and averaged over five heart cycles.
Left Ventricular Mass (LVM) and LVM index were
calculated. Aortic measure-ments were determined
at end-systole and end diastole from the leading
edge of anterior wall of aorta to the leading edge of
the posterior wall of aorta.
Hand Grip Isometric Exercise:
In order to provide aortic measurements over a
range of pressures, all subjects performed isometric
exercise. They were asked to resist inflation of a cuff
of sphygmomanometer while aortic dimensions
and blood pressure were obtained after three
minutes at 50% of maximal hand grip[10].
Statistical analysis:
Continuous variables are summarized as a
mean ± standard deviation (SD). Comparison
between two groups was performed with t - test for
continuous variables and chi-square test for
categorical variables. A p-value < 0.05 was
considered statistically significant and a p-value <
0.01 was considered statistically highly significant.
A stepwise multivariate regression model was used
to identify possible independent variables associated
with reduced aortic root compliance in the
hypertensive patients. The strength of the association
with reduced aortic compliance is presented as 95%
confidence intervals. Potential confounding of
clinical variables was entered as independent
variables.
The validity of the aortic root compliance to
detect coronary artery disease and ischemic heart
disease was assessed by estimating the predictive
indices and Kappa coefficient to determine the
overall agreement with the data obtained from the
coronary angiography and the treadmill exercise
ECG test.
December 2006
Kappa coefficient value (k) = (Observed
frequency of agreement - Expected frequency of
agreement) / (Total observed - Expected frequency
of agreement).
Predictive indices:
True positive (TP), true negative (TN), false
positive (FP) and false negative (FN) were
calculated. Sensitivity = TP/ (TP + FN), specificity =
TN/(TN + FP), positive predictive value = TP/(TP
+ TN), negative predictive value =TN/(TN+TP)
and accuracy = (TP + TN)/(TP + TN + FP + FN).
Simple linear regression (Least-square method)
was used for correlation of the aortic root
compliance and the systolic blood pressure load: Y
= b + aX where, a = slope of the curve and b =
intercept of Y dependent axis (aortic root
compliance) when X independent value (systolic
blood pressure load) became zero.
RESULTS
Clinical characteristics:
As regards the age and gender, there was no
significant difference between both groups in the
study (54.21 ± 7.24 versus 49.9 ± 4.41 years,
respectively, p = NS, 120 (85.7%) versus 25 (83%)
males, p = NS and 20 (14.3%) versus 5 (17%)
females, p = NS) respectively.
There was no significant difference between
both groups regarding a percentage of patients
with history of smoking, diabetes mellitus, and
hypercholesterolemia [46 (32.7%) versus 12 (40%)
patients, p = NS, 29 (20.7%) versus 7 (23%) and 42
(30%) versus 8 (27%) patients, p = NS] respectively.
There was no significant difference regarding the
resting heart rate between both groups (89.25 ± 5.93
versus 78.5 ± 8.72 beat/minute, respectively, p =
NS) but there was a significant increase in the
systolic and diastolic blood pressure in the
hypertensive patients than the normotensives
(177.5 ± 13.41 versus 122.35 ± 8.11 mmHg, and 105.8
± 5.32 versus 76.84 ± 6.18 mmHg, respectively, p <
0.05).
There were 46 patients with a history of
antihypertenisve medication with angiotensin
converting enzyme inhibitors, 32 patients were on
calcium channel blockers, 35 patients were taking
beta-blockers and 27 patients were on angiotensin
receptors blockers.
Exercise ECG test:
There was no significant difference between
both groups in the study as regards the duration of
exercise ECG test, peak heart rate, blood pressure
response during and after exercise and heart rate
recovery after exercise during recovery (p = NS).
There was a significant increased ST - segment
December 2006
KUWAIT MEDICAL JOURNAL
Table 1: Aortic root dimensions before and after isometric
exercise detected by M-mode echocardiography in both
study groups
Variables
At rest before isometric exercise
Aortic Root Area (cm2)
Aortic root Index (cm2/m2)
After 3-minutes hand-grip
isometric exercise
Aortic Root Area (cm2)
Aortic Root Index (cm 2/m2)
Group I
Group II
p-value
8.10 ± 1.32
4.34 ± 0.58
7.26 ± 1.28
3.82 ± 0.64
< 0.05
< 0.05
8.99 ± 1.12
4.64 ± 0.36
8.64 ± 1.07
4.59 ± 0.62
NS
NS
279
Table 2: Compliance of the aortic root in both groups
Variables
∆ A (cm2/m2)
∆ P (mmHg)
C (cm2/m2/mmHg)
Group I
Group II
p-value
0.89 ± 0.08
36.1 ± 4.61
0.025±0.005
1.38 ± 0.18
26.4 ± 3.27
0.052±0.009
< 0.05
< 0.05
< 0.01
C = compliance, ∆A= difference in aortic area, ∆P= difference in systolic blood
pressure
Table 3: Stepwise Logistic Multivariate Analysis of
patients with normal aortic function versus those with
impaired aortic function as regards age, gender, smoking
and hyercholesterolemia
Variables
Age
Gender
Smoking Status
Hypercholesterolemia
Co-efficient
p-value
95% CI
0.4653
0.6301
0.5873
0.1852
< 0.05
< 0.05
< 0.05
< 0.05
1.125 - 4.091
1.021 - 3.505
1.761 - 2.723
1.420 - 2.795
depression in the hypetensive patients than the
normotensive subjects (1.75 ± 0.23 versus 0.42 ± 0.11
mm, respectively, p < 0.05).
Echocardiography:
There was a significant increase in the left
ventricular mass index (LVMI) in both
hypertensive patients and normotensive subjects
(147.3 ± 5.32 versus 119.4 ± 4.68 gm/m2, p < 0.05) .
There was non-significant difference in the left
ventricular systolic function (EF%) between both
groups (62.53 ± 4.26 versus 63.41 ± 2.18%, p = NS),
but there was a significant impaired diastolic
function of the left ventricle in the hypertensives
than normotensives as there was a significant
decrease in the E/A ratio (0.88 ± 0.15 versus 1.51 ±
0.16 respectively, p < 0.05). There was no patient
with signs of aortic root dissection and there were
20 patients with aortic sclerosis and the mean of the
left ventricle/aorta gradient was 24 mmHg. There
was no patient with intramural thrombus or
pericardial effusion.
There was a significant increase in the aortic root
area and the aortic root area index at baseline before
isometric exercise in hypertensive patients than
normotensive subjects ( 8.10 ± 1.32 versus 7.26 ±
1.28 cm2, p < 0.05 and 4.34 ± 0.58 versus 3.82 ± 0.64
cm2/m2, p < 0.05, respectively), but no significant
change in the aortic root area and aortic root area
index after isometric exercise between both groups
in the study ( 8.99 ± 1.12 versus 8.64 ± 1.07 cm2, p =
NS and 4.64 ± 0.36 versus 4.59 ± 0.62 cm2/m2, p =
NS, Table 1).
Fig. 1: Aortic root compliance in the patients with and those without
coronary artery disease
There was a significant increase in the aortic
area after isometric exercise in the normotensive
subjects than before exercise (p < 0.05) but no
significant increase after exercise in the hypertensive
patients (p = NS).
There was a significant decrease in the aortic
root compliance in hypertensive patients than
normotensive subjects (0.025 ± 0.005 versus 0.052 ±
0.009 cm2/m2/mmHg, p < 0.01, Table 2).
There was a significant decrease in the aortic
root compliance in hypertensive patients with
coronary artery disease than those with normal
coronary arteries (p < 0.05, Fig. 1).
Blood pressure load:
Forty-five hypertensive patients had systolic
blood pressure load > 50% and 55 hypertensive
patients had systolic blood pressure load < 50%.
Stepwise logistic multivariate analysis revealed
a significant relation between age, gender, smoking
status and hypercholesterolemia as independent
variables and reduced aortic root compliance in the
hypertensive patients ( r = 0.4653, 0.6301, 0.5873
and 0.1852 and 95% CI = 1.125 - 4.091, 1.021 - 3.505,
280
Feasiblity and Clinical Significance of Echocardiographic Assessment of Aortic Root ....
Table 4: Stepwise Logistic Multivariate Analysis of patients
with normal aortic function versus those with impaired
aortic function as regards antihypertensive drugs
Variables
Beta blockers
ACE inhibitors
AR Blockers
Calcium channel blockers
Co-efficient p-value
0.1653
0.4341
0.3821
0.1659
NS
< 0.05
NS
<0.05
Table 5: Agreement of the treadmill exercise ECG test
and aortic root compliance as regards the prediction of
ischemic heart disease
95% CI
0.524 - 1.091
1.227 - 2.893
0.761 - 1.590
1.428 - 3.236
ACE = angiotensin converting enzyme, AR = angiotensin receptors
December 2006
TTT +ve
Stiff aortic root
30
Compliant aorta
20
Total
50
Kappa Co-efficient value (k) = 0.635
TTT -ve
35
55
90
65
75
140
TTT = treadmill tolerance test
Fig. 3: Correlation between blood pressure load and aortic root
compliance in the hypertensive patients
Fig. 2: The aortic root compliance among the three quintiles of the
hypertensive patients
1.761 - 2.723 and 1.420 -2.795, respectively, p < 0.05,
Table 3). As regards antihypertensive drugs, there
was a significant relation between ACE i n h i b i t o r s
and calcium channel blockers as independent
variables and a reduced aortic root stiffness in
hypertensive patients (R= 0.4341 & 0.1659 and
95%CI = 1.227 - 2.893 & 1.428 - 3.326 respectively, p
< 0.05), but there was no significant relationship
between beta blockers and angiotensin receptors
blockers as independent variables and a reduced
aortic root siffness in the same group (r= 0.1653 &
0.3821 and 95% CI= 0.524 - 1.091 & 0.761 - 1.590
respectively, p = NS, Table 4).
Among the quintiles of the age of hypertensive
patients there was an insignificant difference
regarding the aortic root compliance between the
first and second quintiles (p = NS), but there was a
significant decrease in the aortic root compliance in
the third quintile as compared with the first and the
second quintiles (p < 0.5, Fig. 2).
There was an agreement between data of aortic
root compliance and the treadmill exercise ECG test
to predict the associated ischemic heart disease
with Kappa coefficient value (K) = 0.635, (Table 5)
and with the data of coronary angiography to predict
the associated coronary artery disease with Kappa
coefficient value (K) = 0.761 (Table 6).
There was a significant correlation between
blood pressure load (%) and aortic root compliance
(cm2/m2/mmHg) in hypertensive patients (Y= 0.041X + 0.044, r = -0.873, p < 0.05), and the aortic
root compliance (0.025 cm2/m2/mmHg) of dependent
Y axis corresponded with the blood pressure load
(50%) of independent X axis (Fig. 3).
Table 7 shows the predictive indices for
prediction of the patients with coronary artery
disease and to predict the ischemic heart disease.
DISCUSSION
Stefanadis et al[12] reported that aortic stiffness
and energy loss due to wall viscosity are increased
in hypertensive as compared to the normotensive
patients and diltiazem administration produced an
acute improvement of aortic elastic properties and
a reduction of viscous energy loss. Analysis of the
pressure - diameter relation loop provides a
December 2006
KUWAIT MEDICAL JOURNAL
Table 6: Agreement of the coronary angiography and
aortic root compliance as regards the prediction of
coronary artery disease
Angio +ve
Stiff aortic root
45
Compliant aorta
20
Total
65
Kappa Coefficient value (k) = 0.761
Table 7: Indices for prediction of coronary artery disease
by echocardiographic assessment of aortic root compliance
in all patients group
Angio -ve
10
25
35
281
TP TN FP FN Sen Spec Acc PPV NPV
55
45
100
Prediction of IHD
Prediction of CAD
30
45
55
25
35
10
20 60% 67% 60% 46% 73%
20 69% 71% 70% 81% 56%
Angio = coronary angiography
TP= true positive, TN = true negative, FN = false negative, FP= false positive,
Sen = sensitivity, Spec = specificity, Acc = accuracy, PPV = positive predictive
value, NPV = negative predictive value
valuable insight into aortic mechanics. First, indices
such as distensibility and slope of the pressurediameter loop may be calculated. Second, a study
of the pressure-diameter relationship helps
distinguish between active and passive changes in
aortic elastic properties. The pressure-diameter
relationship for a given subject has a sigmoid
configuration. Movement of the pressure-diameter
loop along this hypothetical sigmoid line suggests
changes in the elastic properties of the aorta due to
changes in aortic pressure alone. In contrast,
shifting of essential modification of the intrinsic
properties of the aorta is also due to non-passive
factors[13]. Third, study of the pressure-diameter
loop provides insights into aortic energetics. In
specific, the area within the loop represents the
energy dissipated to the viscosity of the aortic wall.
Several studies suggest that in hypertension, the
aorta exposed to increased intraluminal pressure
undergoes an increase in mural thickness [14].
Moreover, changes in the structural components of
the arterial wall, including a fall in the ratio of
elastin to collagen, may account for stiffening of the
aorta[15]. In addition, increased smooth muscle
tension is a possible contributor to aortic wall
stiffening in hypertension. Hypertension-induced
endothelial cell dysfunction may also contribute to
alterations of the arterial wall tone, most likely
through impairment of nitric oxide-mediated
vascular smooth muscle relaxation. In advanced
stages of the disease, a further factor that reduces
arterial compliance is the deposition of calcium[16].
The amount of severity of atherosclerosis in the
coronary bed shows a positive correlation with the
degree of atherosclerosis in the aorta or other major
arterial branches [17]. Atherosclerotic changes in
arterial wall have been shown to include smooth
muscle cell proliferation, deposition of lipid and
accumulation of collagen, elastin and proteoglycans.
Changes in the ratio of collagen to elastin have been
known to structurally affect the elastic behavior of
arterial walls.
Our finding of an impaired aortic root compliance
in hypertensive patients with coronary artery
disease is in keeping with previous smaller
studies[18]. Another study has shown that proximal
aortic stiffness is increased progressively with the
number of diseased coronary blood vessels in
patients investigated after myocardial infarction[19].
Only 100 patients were known to have undergone
coronary angiography in the course of their routine
clinical management and out of these only 40
patients had normal coronary arteriography, 10
patients had positive exercise test which may be
due to other causes (e.g., coronary spasm or
mirovascular disease), and this seems unlikely to
have seriously confounded our results.
We found that the age, gender, smoking status
and hyper cholesterolemia were independent
variables to increase the risk of the aortic stiffness
and this is in an agreement with other studies[19-22].
An increase in the stiffness of the aorta with
elevated plasma lipids has been related to the
increased endothelium vasoactivity and decreased
vasa vasorum flow. Cholesterol may enhance
arterial stiffening, but this process is modulated by
other risk factors for CAD[20].
Smoking is a major and independent risk factor
for cardiovascular morbidity and mortality [21].
Many underlying mechanisms have been proposed
for the hazardous effects of smoking, including
promotion of atherogenesis, unfavourably changed
lipid profile, increased blood viscosity, alterations
in platelet function and promotion of thrombosis
and enhanced adrenergic activity. Previous studies
have shown that smoking also induces coronary
artery vasoconstriction and affects arterial elastic
properties unfavorably, increasing stiffness of both
muscular and elastic arteries.
We found that the angiotensin converting
enzyme inhibitors and calcium channel blockers
were independent variables for decreasing the risk
of the aortic stiffness and this is in agreement with
other studies[23,24]. Diltiazem has an active effect on
the elastic properties of the aorta due to direct
relaxation of the aortic smooth muscle and increase
in the vasodilatory capacity of the vasa vasorum of
the aortic wall which is decreased in chronic
hypertension[3].
282
Feasiblity and Clinical Significance of Echocardiographic Assessment of Aortic Root ....
Methodological consideration:
The method used in the present study provides
reliable, non- invasive and valid determination of
the aortic root function in hypertensive patients
and can be reproduced in the hypertension clinic
but the invasive methods using the high fidelity
diameter measuring device and the catheter-tip
micromanometer measuring aortic pressure has
been validated and proved to be accurate and safe[3].
The variability of echocardiography determined
indices of aortic stiffness has been found previously
to be < 10% for inter-observer comparisons. For
measurements repeated at 4-week intervals, intraobserver variability was < 10%[3,17]. In our study
only one cardiologist performed echocardiographic
assessment once. Therefore it is difficult to assess
inter-observer and intra-observer variability.
Department, Farwania hospital, for his advice and
help in the preparation of this manuscript, and Dr
Walid Ahmad Mostafa and Dr Ahmad Muneer,
Cardiologists of Medicine Department, Farwania
hospital, for their valuable help.
REFERENCES
1.
2.
3.
4.
Limitations of the study:
1. Relatively small number of patients.
2. The study was not blind to the cardiologist
performing the echocardiography.
3. Blood pressure was recorded indirectly by
cuff sphygmomanometer.
4. Coronary vasomotor reactivity was not
included in the design of the study.
5. Pregnant women were not included in the
study to avoid the confounding effect of the
estrogen on the elasticity of the aorta. The
aorta is more dilated and more compliant
during normal human pregnancy, especially
in multi-parus women [25].
6. Hypertensive patients with end-organ damage
were not included in the study.
CONCLUSION
Aortic root compliance is compromised in
hypertensive patients as compared with normotensive
subjects and it can be considered as a marker for
prediction of coronary artery disease. Aortic root
compliance is a precise estimate for risk
stratification in the management of hypertensive
patients as the serial evaluation of the aortic root
stiffness allows early detection of pathologic
acceleration of atherosclerotic complications.
ACKNOWLEDGMENT
With great honor, we thank Dr Saleh Ali AlEnezi, Chairman of Medicine Department and Dr
Ahmad Al-Dousary, Consultant Endocrinologist,
Medicine Department, Farwania hospital for their
kind cooperation and continuous support accorded
to this study. We also thank Mrs Delfeyanoum
Hussain and Mrs Suzan of the Non-Invasive
Cardiac Laboratory, Farwania hospital, for their
cooperation in preparation of patients, Dr Samuel
Cherian,
Consultant
Physican,
Medicine
December 2006
5.
6.
7.
8.
9.
10.
11.
12.
13.
14.
15.
16.
Ohtsuka S, Kakihana M, Watanabe H, SugishitaY.
Chronically decreased aortic distensibility causes
deterioration of coronary perfusion during increased left
ventricular. J Am Coll Cardiol 1994; 24:1406-1414.
Kelly RP, Tunin R, Kass DA. Effect of reduced aortic
compliance in cardiac efficiency and contractile function of
in situ canine left ventricle. Circ Res 1992; 71:490-502.
Stefanadis C, Dernellis J, Vlachopoulos C, Tsioufis C,
Tsiamis E, Toutouzos K, Pitsavos C, Toutouzas P. Aortic
function in hypertension determined by pressure-diameter
relation. Effects of diltiazem. Circulation1997; 96:1853 -1858.
Pitsavos C, Stefanadis C, Toutouzas P. Aortic structure and
function in arterial hypertension. In: Boudoulas H,
Toutouzas P, Wooley CF, editors. Functional abnormalities
of the aorta. Armonk, NY: Futura Publishing; 1996, p 333342.
Roy CS. Elastic properties of the arterial wall. J Physiol
1980; 3:125-159.
Stefanadis C, Stratos C, Boudoulas H, Koureouklis C,
Toudoulas P. Distensibility of the ascending aorta:
comparison of invasive and non-invasive techniques in
healthy men and in men with coronary artery disease. Eur
Heart J 1990; 11:990-996.
Bouthier JD, De Luca N, Safar ME, Simon AC. Cardiac
hypertrophy and arterial distensibilty in essential
hypertension. Am Heart J 1985; 109:1345-1352.
O’Brien ET, Fitzgerald D, O’Malley K. Comparison of clinic,
home and ambulatory blood pressure measurement. J
Ambulatory Monitoring 1988; 1:285-291.
Lauer MS, Francis GS, Okin PM, Pashkow FJ, Snader CE,
Marwick TH. Impaired chronotropic response to exercise
stress testing as a predictor of mortality. JAMA 1999;
281:524-529.
Hopkins KD, Lehmann ED, Gosling RG. Aortic compliance
measurements: A non-invasive indicator of atherosclerosis?
Lancet 1994; 343:1447-1448.
Deveroux RB, Reichek N. Echocardiographic determination
on left ventricular mass in man: anatomic validation of the
method. Circulation 1977; 55:613-618.
Stefanadis C, Karayannacos PE, Boudoulas H, Stratos C,
Vlachopoulos C, Dontas I, Toutouzas P. Medial necrosis and
acute alterations in aortic distensibility following removal
of the vasa vasorum of canine ascending aorta. Cardiovasc
Res 1993; 27:951-956.
Stefanadis C, Vlachopoulos C, Karayannacos PE, Boudoulas
H, Stratos C, Filippides T, Agapitos M, Toutouzas P. Effects
of vasa vasorum flow on stucture and function of the aorta
in experimental animals. Circulation 1995; 91:2669-2678.
Pearson AC, Guo R, Orsinelly DA, Binkley PF, Pasiersky TJ.
Transesophageal echocardiographic assessment of the
effects of age, gender and hypertension on thoracic aortic
wall size, thickness and stiffness. Am Heart J 1994; 128:344351.
Isnard RN, Pannier BM, Laurent S, London GM, Diebold B,
Safar ME. Pulsatile diameter and elastic modulus of the
aortic arch in essential hypertension: a noninvasive study. J
Am Coll Cardiol 1989; 13:399-405.
Beltz GG. Elastic properties and windkessel function of the
human aorta. Cardiovasc Drugs Ther 1995; 9:73-83.
December 2006
KUWAIT MEDICAL JOURNAL
17. Stefanadis C, Dernellis J, Tsiamis E, Stratos C, Diamantopoulos
L, Michaelides A, Toutouzas P. Aortic stiffness as a risk
factor for recurrent acute coronary events in patients with
ischaemic heart disease. Eur Heart J 2000; 21:390-396.
18. Gatzka CD, Cameron JD, Kingwell BA, Dart AM. Relation
between coronary artery disease, aortic stiffness and left
ventricular structure in a population sample. Hypertension
1998; 32:575-578.
19. Hirai T, Sasayama S, Kawasaki T, Yagi S. Stiffness of systemic
arteries in patients with myocardial infarction. A
noninvasive method to predict severity of coronary
atheroscelrosis. Circulation 1989; 80:78-86.
20. Dart AM, Lacombe F,Yeoh JK, Cameron JD, Jennings GL,
Laufer E, Esmore DS. Aortic distensibility in patients with
isolated hypercholesterolemia, coronary artery disease or
cardiac transplant. Lancet 1991; 338:2891-2897.
21. Pitsavos C, Toutouzas K, Dernellis J, Skoumas J,
Skoumbourdis E, Stefanadis C, Toutouzas P. Aortic stiffness
22.
23.
24.
25.
283
in young patients with heterozygous familial hypercholesterolemia. Am Heart J 1998; 135:604-608.
Stefanadis C, Tsiamis E, Vlachopoulos C, Stratos C,
Toutouzas K, Pitsavos C, Marakas S, Boudoulas H,
Toutouzas P. Unfavorable effect of smoking on the elastic
properties of the human aorta. Circulation 1997; 95:31-38.
Shimamoto H, Shimamoto Y. Lisinopril reversed left
ventricular hypertrophy through improved aortic
compliance. Hypertension 1996; 28:457-46.
Stefanadis C, Stratos C, Boudoulas H, Vlachopoulos C,
Kallikazaros I, Toutouzas P. Distensibility of the ascending
aorta in coronary artery disease and changes after
nifedipine administration. Chest 1994; 105:1017-1023.
Giraud GD, Morton MJ, Wilson RA, et al. Effects of estrogen
and progestin on aortic size and compliance in
postmenopausal women. Am J Obstet Gynecol 1996;
174:1708 -1717.
KUWAIT MEDICAL JOURNAL
December 2006
Original Article
Prevalence and Factors Associated with Obesity and
Treatment of Blood Pressure among Kuwaiti Hypertensive
Patients in a Primary Health Care Clinic
Nadia Yousef Al-Mahmoud
Ehqaqi Primary Health Care Clinic (Daiya Clinic), Kuwait
Kuwait Medical Journal 2006, 38 (4): 284-286
ABSTRACT
Objectives: To determine the prevalence of obesity
among adult hypertensive patients and to investigate
associated factors and the differences in drug doses at the
Daiya primary care clinic in Kuwait
Design: Cross-sectional study
Method: Two hundred hypertensive Kuwaiti patients on
antihypertensive medication and attending the Daiya
clinic during a period of six months between January and
June 2004 were included in the study.
Results: A high prevalence of obesity (68%) was seen
among hypertensive patients. The multiple logistic
regression analysis showed that the significant associated
factors were non- compliance with diet (p = 0 .006) and
age (< 65, p = 0.002). Factors such as intake of evening
snacks and family history of obesity were not found to be
significantly associated. Obese patients needed more
than one drug to control their blood pressure.
Conclusion: There is a high prevalence of obesity among
hypertensive patients. Hence, intensive programs are
recommended to control their obesity.
KEYWORDS: body mass index, hypertension, obesity, primary care
INTRODUCTION
Obesity, according to WHO, is defined as Body
Mass Index (BMI = weight in kilograms divided by
height in meters squared) ≥ 30 kg/m2 and overweight
as BMI ≥ 25 kg/m2[1]. Obesity, characterized by
storage of additional body fat, develops when
energy intake exceeds energy expenditure [2].
Epidemiological studies show that about 55% of US
adult population is overweight and 22% is obese.
In the last two decades obesity has increased by
more than 30% in USA [1]. The prevalence of obesity
in Kuwait has increased by 15.4% between 1980-81
and 1993-94 among Kuwaiti men due to
modernization, affluence and concomitant changes
like sedentary life style [3]. Prevalence of overweight
and obesity also increased among both gender in
Kuwait between 1980 - 81 and 1993 - 94. The rate of
temporal changes in BMI and obesity were higher
by comparison in Kuwait than in selected other
countries[4,5].
Obesity, especially upper body fat distribution
is an independent risk factor for the development
of hypertension[6-9]. Hypertension is defined as
blood pressure ≥ 140/90 mmHg with or without
antihypertensive medication [10]. Recent studies
showed that both systolic and diastolic blood
pressure increases in a linear manner over the
whole range of BMI or waist circumference[11-12].
Obesity being one of the risk factors and
determinant of poor BP control, it was thought
necessary to study the factors associated with
obesity among hypertensive patients. Weight
reduction is one of the most effective non pharmacological approach to BP control[7].
Hypothesis
Majority of hypertensive patients are obese.
Factors associated with obesity are lack of exercise
and poor diet compliance. More number of drugs
are needed to control BP among obese patients.
METHODOLOGY
A cross - sectional study was undertaken at the
Daiya (Al - Ehqaqi) primary care clinic in Kuwait
during a period of six months between January and
June 2004. The study included 200 consecutive
Kuwaiti hypertensive patients who attended the
Daiya primary health care clinic for monthly follow
- up. They were among 300 patients registered in
the clinic. Non Kuwaitis were excluded.
A structured questionnaire was either self administered or assisted by the author in illiterate
patients. The questionnaire included the characteristics
of the patients (e.g., age, gender, onset of hypertension,
Address correspondence to:
Dr. Nadia Yousef Al-Mahmoud, Head, Ehqaqi Primary Health Care Clinic (Daiya Clinic), Shamiya, P.0. Box 12364, Kuwait 71654. Tel & Fax:433
5653
December 2006
KUWAIT MEDICAL JOURNAL
Table 1: Comparison of associated factors with levels of
body mass index (BMI, kg/m 2)
Factors
BMI < 30 (n=63)BMI ≥ 30 (n=135) p- (*)
n
(%)
n
(%) value
Exercise
Does exercise
No exercise
Snacks in the morning
Eats
Does not eat
Snacks in the evening
Eats
Does not eat
Diet compliance
Is compliant
Not compliant
Family history of obesity
Had family history
No family history
Age
< 65
≥ 65
Mean age ± 13.2 yrs
Mean age at onset of
hypertension ± 13.0 yrs
0.348
19 (30.2)
44 (69.8)
32
102
(23.9)
(76.1)
24 (38.1)
39 (61.9)
62
72
(46.3)
(53.7)
12 (19.0)
51 (81.0)
56
79
(41.5)
(58.5)
41 (56.1)
22 (34.9)
52
83
(38.5)
(61.5)
9 (14.3)
54 (58.7)
40
93
(30.1)
(69.9)
31 (49.2)
32 (50.8)
102
33
58.2
(75.6)
(24.4)
0.281
0.002
<0.001
0.017
<0.001
50.9
*p-values were generated using chi - square test, student’s and t-test to compare
means.
treatment, diet compliance, exercise and family
history of obesity). BP was measured using a
mercury sphygmomanometer and recorded in the
file (taking the last three readings in file on three
separate visits at least one month apart). Thereafter,
patients’ weight and height were taken by the
author, used physician Balance BEAM Scale and
BMI was calculated.
The data was entered and analyzed in SPSS
(Statistical Package for Social Sciences). Chi-square
test was used for the categorical variables and pvalue < 0.05 was considered as significant. Factors
associated with obesity among hypertensive
patients were identified using logistic regression
multivariate analysis.
RESULTS
The mean age of patients in the study group was
58.16 ± 13.2 years, mean age at onset of
hypertension 51 ± 13.0 years and mean BMI was
32.44 ± 5.50 kg/m2. It was also found that the BP
was controlled in 77% patients.
The patients were classified into two groups
based on their BMI. Those with a BMI ≥ 30 were
considered obese while those with a BMI ≤ 30 were
non - obese. According to this classification, the
prevalence of obesity among hypertensive patients
in this sample was 68%.
There was no apparent difference in gender
among the low BMI patients, but among the high
BMI, there seemed to be more females (75%) than
285
Table 2: Factors associated with obesity among hypertensive
patients as identified by the logistic regression analysis
Variable
Adjusted odds ratio
Evening snack
No (control)
Yes
Diet compliance
Yes (control)
No
Family history of obesity
No (control)
Yes
Age (in years)
< 65
≥ 65
95% C I p-value
2.115
0.98 - 4.566
0.056
2.581
1.316 - 5.065
0.006
1.678
0.712 - 3.953
0.236
2.922
1.48 - 5.767
0.002
Dependent variable (BMI < 30 kg/m 2 = 0 ,BMI ≥ 30 kg/m 2 = 1)
95% CI = 95% confidence interval for adjusted odds ratio
males (60%). Table 1 describes comparison of
associated factors with level of BMI. It was
observed that eating snacks in the evening was
significantly associated with obesity (41% obese
versus 19% non-obese). Non-compliance to a
proper prescribed diet showed that 61.5% were
obese compared to 34.9% non-obese. Patients in the
age group < 65 years were significantly associated
with obesity (75.6%). Doing exercise and eating
morning snacks had no significant association with
obesity in this study
A multivariate analysis was done to see the
combined effect of the significant factors on obesity.
Table 2 describes factors associated with obesity
among hypertensive patients as identified by the
logistic regression analysis. This shows that non compliance to prescribed diet (p = 0.006) and age
< 65 years (p = 0.002) were significant.
A significant association was found between
doing exercise and blood pressure control regardless
of obesity. Amongst those who did exercise, 88.2%
had their BP controlled whereas in those not
exercising, only 74% had their BP controlled.
Among the non- obese, about 73% patients
could manage to control their BP with only one
drug as opposed to about 52% in the obese group
which was statistically significant.
DISCUSSION
The prevalence of obesity among hypertensive
patients was 68% in our study group. This indicates
that obesity is a major risk factor for the
development of hypertension as indicated by
previous studies [1,6,9-13]. As obesity is independently
associated with hypertension, there is a strong need
to address the problem among hypertensive
patients. A previous study in Kuwait reported
women more obese than men[14]. This was also
observed in our study.
286
Prevalence and Factors Associated with Obesity and Treatment of Blood Pressure among .... December 2006
As seen in this study, compliance to prescribed
diet and not eating snacks in the evening had a
significant direct association with non-obesity. This
should be considered as a significant non pharmacological measure to control blood pressure
[7,9-10]
.
The current study showed that significant
proportion of obese people needed two or more
drugs to control their blood pressure which again
calls for losing weight as an important measure. As
mentioned in some other studies, weight loss can
help decrease the number and dosage of drugs
which can reduce side-effects and treatment
costs[7,9,12,14].
In the multivariate analysis, it was found that
age factor is a strong predictor of obesity and this is
high among the middle age group. The mean age of
onset of hypertension in the study group was 51
years. Therefore, it can be suggested that more
attention should be given to this age group by the
GPs as regards their health education about obesity
related hypertension[9,12,15,16].
Exercise was found to play a significant role in
the control of BP. Therefore, reinforcing the need to
exercise is a very important part of hypertension
management[9,10,17-19].
The current study thus reinforces the obvious
fact that obesity is one of the prime predisposing
factors for hypertension and that all necessary
measures to control obesity will facilitate any
treatment for this condition.
3.
4.
5.
6.
7.
8.
9.
10.
11.
12.
13.
14.
15.
ACKNOWLEDGEMENTS
I would like to thank Dr Madhavan Ravindran,
Dr Mohamed Mosa, Dr Manal Muter and Mrs. Indu
Menon for their support
17.
REFERENCES
18.
1.
2.
Atkinson RL. A 33- year old women with morbid obesity.
JAMA2000; 283:90-94.
Hamann A, Sharma AM. Genetics in obesity and obesity
related hypertension. Seminars in Nephrology 2002; 22:100104.
16.
19.
Al-Isa AN. Temporal changes in body mass index and
prevalence of obesity among Kuwaiti men. Annals of
Nutritional Metabolism 1997; 41:307-749.
Al-Isa AN. Body mass index and prevalence of obesity
among Kuwaitis. European Journal of Clinical Nutrition
1997; 51:743-749.
Al-Isa AN. Changes in body mass index and prevalence of
obesity among Kuwaitis 1980-1994. International Journal of
obesity 1997; 21:1093-1099.
Rocchini AB. Obesity hypertension. American Journal of
Hypertension 2002; 15:505-525.
Zhang R, Thakur V, Morse S, Reisin E. Renal and
cardiovascular considerations for the non-pharmacological
and pharmacological therapies of obesity - hypertension.
Journal of Human Hypertension 2002; 16:819-827.
Bell AC, Adair LS, Popkin BM. Ethnic differences in the
association between body mass index and hypertension.
American Journal of Epidemiology 2002; 155:346-353.
Al-Turki AY. The prevalence of overweight and obesity
amongst hypertensive and diabetic adult patients in
primary health care. Saudi Medical Journal 2000; 21:340343.
MacKnight JM. Exercise consideration in hypertension,
obesity and dyslipidemia. Cinical Sports Medicine 2003;
22:101-121.
Engeli S, Sharma AM. Emerging concepts in the pathophysiology and treatment of obesity-associated hypertension.
Current opinion in Cardiology 2002; 17:355-359.
Leiter LA, Abbot D, Campbell RC, Mendelson R, Ogilive
RI, Chockalingam A. Recommendations on obesity and
weight loss. Can Med Assoc J 1999; 1600:S7-S11.
Hall JE. The kidney, hypertension, and obesity.
Hypertension 2003; 41:625-633.
Saito I, Murata k, Hirose H, Tsujika M and Kawabe H.
Relation between blood pressure control, body mass index
and intensity of medical treatment. Hypertension Research
2003; 26:711-715.
Al-Isa AN. Prevalence of obesity among adult Kuwaitis: a
cross -sectional study. Internat J Obes 1995; 19:431-433.
Al-Isa AN. Changes in body mass index and prevalence of
obesity among adult Kuwaiti women attending health
clinics. Ann Saudi Med 1997;17:307-311.
Campbell RC, Burgess E, Taylor G, et al. Lifestyle changes to
prevent and control hypertension: Do they work? Can Med
Assoc J 1999; 160:1341-1343
Cleroux J, Feldman RD, Petrella RJ. Recommendations on
physical exercise training. Can Med Assoc J 1999; 160: s21s27.
Davy KP, Hall JE. Obesity and hypertension: two epidemics
or one? Am J Physiol Regul Integr Comp Physiol 2004; 286:
R 803- R 813.
December 2006
KUWAIT MEDICAL JOURNAL
Original Article
Factors Influencing Outcome of Congential Diaphragmatic
Hernia
Bhaskar Ramgopal Gupta
Department of Pediatrics and Neonatology, Special Care Baby Unit, Khoula Hospital, Muscat, Sultanate of Oman
Kuwait Medical Journal 2006, 38 (4): 287-291
ABSTRACT
Objective: To assess the presentation of congenital
diaphragmatic hernia and to analyze the outcome of
such babies according to the the prognostic indicators in
a neonatal intensive care unit
Design: Retrospective
Material and Method: All cases of congenital diaphragmatic
hernia admitted to the neonatal intensive care unit at
Khoula Hospital, Muscat, Sultanate of Oman from
February 1994 to February 2001 were included in the
study. The antenatal factors, presentation, resuscitation
and the management of these babies were reviewed and
their survival according to prognostic indicators compared
with similar cases in literature.
Results: A total of 10 cases of congenital diaphragmatic
hernia were admitted during this seven year period with
an overall mortality of 80%.
Gestational age ranged from 33 weeks to full term. Eight
(80%) babies had severe birth asphyxia needing
intubation and ventilation soon after birth and had 100%
mortality.
Two (20%) babies had mild birth asphyxia and presented
after eight hours of life and had 100% survival. Five
(50%) had polyhydramnios and three (30%) had
associated anomalies. Ventilation index was < 1000 in
three ( 30%) babies with a mortality of 33.3% and > 1000
in seven (70%) babies with 100% mortality.
Two ( 20%) babies operated after five days had 100%
survival. Severe birth asphyxia, metabolic acidosis, hypoxia,
hypercarbia and early presentation of diaphragmatic
hernia had high mortality. Associated persistent pulmonary
hypertension (PPHN) and pneumothorax had 100%
mortality. Survival was seen in those two babies who had
good prognostic factors and were operated after
stabilization.
Conclusion: Compared to other neonatal intensive care
units, mortality rate in our unit remains high in neonates
presenting with congenital diaphragmatic hernia. This is
due to lack of newer modes of ventilation, nitric oxide
therapy and extracorporeal membrane oxygenation
(ECMO).
KEY WORDS: congenital diaphragmatic hernia, prognostic indicators, ventilation index
INTRODUCTION
Congenital diaphragmatic hernia (CDH) is a
disorder characterized by failure of the pleural and
peritoneal canal to close approximately at eight
week of gestation. This leads to displacement of
the abdominal contents into the thoracic cavity
resulting in pulmonary hypoplasia due to
compression of the developing lungs by the
viscera. Hernias through the posterolateral aspect
of the diaphragm ( Foramen of Bochdalek) account
for approximately 80% of hernias, and hernias on
the left side are five times more common than on
the right side.
With the increased use of obstetric ultrasound,
prenatal diagnosis of these hernias is common.
Neonates present with asphyxia, respiratory
distress, cyanosis and scaphoid abdomen. Those
who develop respiratory failure within the first six
hours of life have the highest mortality. Despite the
advances in neonatal intensive care and ventilation
the mortality remains frustratingly high.
Various prognostic indicators have been
suggested for survival of babies with CDH. These
include birth weight, APGAR scores, age of
presentation, associated congenital anomaly and
ventilatory parameters like ventilation index,
pCO2, pO2 and oxygenation index. Other indicators
are complications like pneumothorax, persistent
pulmonary hypertension (PPHN) and also types of
therapies used like hyperventilation, drugs and
extracorporeal membrane oxygenation (ECMO).
In the past, babies with CDH were rushed
immediately to the operating room without
stabilization, but all the recent practice is to
stabilize these patients first especially with the use
of ECMO which has lead to significant improvement
Address correspondence to:
Dr Bhaskar Ramgopal Gupta, M.B.B.S,M.D. (Pediatrics), Pediatrician & Neonatologist, Yiaco Apollo Medical Center, Post Box 24098, Safat
13101, Kuwait. Tel No: 00965-5648040, Ext 108, Fax: 00965-5646070, E-mail: [email protected]
288
Factors Influencing Outcome of Congential Diaphragmatic Hernia
Table 1: Antenatal and perinatal factors affecting mortality
in babies born with CDH
No. of Babies
n (%)
1. Type of delivery
Spontaneous vaginal delivery
Emergency LSCS
2. Sex
Male
Female
3. Gestation
Preterm
Term
4. Birth Weight
< 2.5 kg
> 2.5 kg
5. Associated anomalies
6 Antenatal Ultrasound
Polyhydramnios
Diaphgrmatic hernia
Not done
Table 2: Factors influencing mortality in diaphragmatic
hernia
Mortality
n (%)
8 (80)
2 (20)
6 (75)
2 (100)
6 (60)
4 (40)
4 (66.6)
4 (100)
2 (20)
8 (80)
2 (100)
6 (75)
2 (20)
8 (80)
3 (30)
2 (100)
6 (75)
3 (100)
5 (50)
3 (30)
2 (20)
5 (50)
3 (100)
1 (50)
in outcome. Now the emphasis is on ventilatory
strategies that minimize airway pressure and
reduce barotrauma to the severely hypoplastic
lungs.
This retrospective analysis over a period of
seven years of all babies with CDH born at Khoula
Hospital Muscat, Sultanate of Oman was undertaken
at a neonatal intensive care unit (NICU) where no
ECMO or pediatric surgical facilities were available.
The aim was to determine the presentation of
congenital diaphragmatic hernia and its outcome in
these babies.
METHODS
All babies born at Khoula Hospital from
February 1994 to February 2001 with the diagnosis
of CDH and admitted to the NICU were included
in the study. Their case notes were retrieved and
analyzed for the antenatal presentation and the
postnatal outcomes.
All babies were ventilated with pressure
controlled, timed cycled positive pressure ventilators
(Bear Cub, Sechrist and Drager ventilators). The sex
of the baby, gestation, type of delivery, antenatal
ultrasound for congenital anomalies, initial
APGAR, the need for resuscitation and their
anthropometric measurements were noted.
All the babies were shifted soon after birth to the
NICU and the age of presentation of the
diaphgrmatic hernia was noted. Oxygen needs and
ventilatory requirements like maximum pressure,
oxygen and ventilation index was calculated.
Arterial blood was collected and analyzed by
Blood gas analyzer for initial pH, pO2, pCO2 and
base excess. Ventilation and electrolytes monitoring
December 2006
1. Birth Asphyxia
Severe
Mild
2. Time of presentation
Soon after birth
> 8 hours after birth
3. Site of hernia
Left
Right
4. Associated PPHN
5. Pneumothorax
No. of Babies
n (%)
Mortality
n (%)
8 ( 80)
2 (20)
8 (100)
0 (0)
8 (80)
2 (20)
8 (100)
Nil (0)
8 (80)
2 (20)
8 (80)
3 (30)
7 (87)
1 (50)
8 (100)
3 (100)
of all these babies during their stay in the NICU
was done according to the unit protocols. The
criteria for conventional ventilation included
severe persistent metabolic acidosis, pO2 < 60
mmHg and progressively rising pCO2 > 60 mmHg.
All babies had a peripheral arterial line for blood
sampling. Monitoring of these babies was done by
continuous recording of heart rate, temperature,
pulse oximetry, respiratory rate and blood pressure
recordings on a Hewlett Packard cardiac monitor.
Repeated blood gas analysis according to the
changes in ventilation and complete blood counts,
electrolyte and blood sugar monitoring was done.
Additional management of some babies with
PPHN consisted of applying modalities like use of
drugs such as tolazoline and prostacyclin. The
response to treatment and complications of
ventilation like associated pneumothorax was
noted and final outcome was analyzed.
As the NICU at Khoula Hospital had no facilities
for pediatric surgery, the neonates were stabilized
and then shifted on a transport ventilator ( D r a g e r )
to a tertiary care NICU at the Royal Hospital
where they were managed by a team of pediatric
surgeons and neonatologists. The time of transfer,
operative management and associated mortality
was also assessed.
All these data was analyzed for the incidence of
CDH during these seven years, its presentation and
outcome.
RESULTS
During the seven year period from February
1994 to February 2001, there were a total of 30,157
live-born babies at Khoula hospital out of which ten
had CDH. Six (60%) were female and four (40%)
male. Gestational ages of these babies ranged from
33 weeks to full term. Two out of them were preterm.
Eight (80%) babies were born by normal vaginal
delivery and two (20%) by emergency LSCS.
Polyhydramnios was noted in five (50%),
December 2006
KUWAIT MEDICAL JOURNAL
Table 3: Initial blood gas parameter and mortality in
congenital diaphragmatic hernia
No. of Babies
n (%)
1 pH
<7
7 (70)
7 - 7.2
2 (20)
> 7.2
1 (10)
2. pO2
30-60 mm of Hg
8 (80)
> 60 mm of Hg
2 (20)
3. pCO 2
> 60 mm of Hg
6 (60)
< 60 mm of Hg
4 (40)
4. Severe metabolic acidosis
8 (80)
5. Ventilation Index (MAPx Respiratory rate)
< 1000
3 (30)
> 1000
7 (70)
Table 4: Interventions and mortality in diaphragmatic
hernia
Mortality
n (%)
7 (100)
1 (50)
Nil (0)
8 (100)
Nil (0)
6 (100)
2 (50)
8 (80)
1 (33.3)
7 (100)
diaphragmatic hernia noted antenatally in three
(30%) and associated anomalies in the form of
dysmorphic features and cardiovascular anomalies
in three (30%) babies (Table 1).
Eight (80%) babies had severe birth asphyxia
needing intubation and ventilation soon after birth
with 100% mortality. Two (20%) babies had mild
birth asphyxia and presented late (after 8 hours)
and had 100% survival.
Left sided hernia was seen in eight (80%) cases
out of which seven (87%) died and right sided
hernia in two cases out of which one (50%) died.
PPHN was present in eight (80%) cases with 100%
mortality and pneumothorax in three cases with
100% mortality (Table 2).
Conventional ventilation was used in all babies
using Bear Cub, Sechrist or Drager ventilators and
drugs like tolazoline and prostacyclin were used in
four (40%) babies with 100% mortality.
Blood gas analysis showed that seven (70%)
babies with an initial pH < 7 had 100% mortality.
Two babies (20%) had a pH between 7-7.2 with 50%
mortality and one baby (10%) with a pH > 7.2
survived. Eight babies (80%) with an initial pO2 of
30-60 mmHg had 100% mortality. Those with a pO2
> 60 mmHg (2 babies, 20%) survived. Six babies
(60%) with a pCO2 > 60 mmHg died whereas four
babies (40%) with a pCO2 < 60 mmHg showed a
50% mortality. Severe metabolic acidosis with base
excess of more than -15 was seen in eight (80%)
cases with 100% mortality. Ventilation Index, a ratio
of mean airway pressure x respiratory rate was <
1000 in three (30%) babies with a mortality of 33.3%
and > 1000 in seven (70%) cases with a mortality of
100% (Table 3).
Six (60%) babies were stabilized and transferred
to a tertiary care unit with a pediatric surgical
service and four (40%) were operated. Two (20%)
289
No. of Babies
n (%)
1. Age at ventilation
Soon after birth
> 8 hrs after birth
2. Type of ventilation
Conventional
Conventional with tolazoline/
prostacyclin
3. Transfer to tertiary care hospital
Transferred
Not transferred
4. Operated
5. Age of surgery
< 5 days
> 5 days
Overall Mortality
Mortality
n (%)
8 (80)
2 (20)
8 (100)
Nil (0)
10 (100)
8 (80)
4 (40)
4 (100)
6 (60)
4 (40)
4 (40)
4 (66.6)
4 (100)
2 (50)
2 (20)
2 (20)
10 (100)
2 (100)
Nil (100)
8 (80)
were operated within five days of birth and both
died while the other two operated later survived.
Four (40%) babies could not be transferred as they
could not be stabilized and died at Khoula
Hospital. PPHN was present in eight (80%) cases
with 100% mortality and pneumothorax in three
(30%) cases with 100% mortality. Conventional
ventilation was used in all babies and drugs like
tolazoline and prostacyclin were used in four (40%)
cases with 100% mortality. The overall mortality
was eight (80%) and those who survived presented
late and were operated upon after the 1st week of
life (Table 4).
DISCUSSION
The infant born with CDH presents a challenge
and remains one of the most complex patients to
manage. Pulmonary hypoplasia and immaturity of
the lung are well-recognized definitive limitations
leading to high mortality rates [1]. Congenital
diaphragmatic hernia is a well-known condition for
almost 200 years but its treatment strategy has
changed during the past few decades. Despite these
improvements the mortality rates remain frustratingly
high (> 50%), especially for those presenting in the
first six hours of birth[2,3].
We analyzed our experience with this condition
over the last seven years in our NICU where no
facilities for high frequency ventilation or ECMO
were available. After the initial ventilation and
stabilization these babies had to be transferred to a
pediatric surgical unit in other hospital.
The incidence of congenital diaphragmatic
hernia in our unit was 1:3000 live births which corelates well to that reported in the literatur e.
National Maternity Hospital in Dublin, Ireland
reported an incidence of 1:2107 after a review of
290
Factors Influencing Outcome of Congential Diaphragmatic Hernia
99,000 patients[4]. Left sided hernia was seen in 80%
cases which is similar to our finding[5]. Gestational
age analysis revealed that most of our babies (80%)
were term babies. Polyhydramnios was seen in 50%
cases. Three of our babies were diagnosed
antenatally as cases of CDH and were referred for
delivery to a center with pediatric surgical facilities.
But they came in labor at our institute and the
babies had 100% mortality. In most centers,
antenatal diagnosis with sonography is accurate in
88-94% cases as reported by Bell et al who also
found polyhydramnios in most of their cases[6].
Three (30%) babies had associated anomalies in
the form of dysmorphic features of Trisomy 18,
hydrocephalus and ventricular septal defect with
100% mortality in this group. Associated anomalies
are present in 35% of cases out of which cardiac
lesions predominate and infants with associated
anomalies have a low APGAR, lower pO2 and poor
prognosis[7]. The Iowa city birth defects registry
noted that 28% of babies with CDH had associated
anomalies like meningocele, encephalocele,
hydrocephalus, ventricular septal defect, vascular
rings, trisomy 13 and 18, omphalocele and had poor
survival rates (5%) [8].
Eight (80%) babies presented soon after birth
and had severe birth asphyxia needing intubation.
They were ventilated soon after birth with
conventional ventilation at high parameters. This
group with early presentation and low APGAR had
100% mortality. Two (20%) babies presented after
eight hours and survived. The CDH study group
from the department of surgery, University of
Texas, Houston estimated the disease severity in
first five minutes of life. Survival data on 322
consecutive live-born infants with CDH were
collected from 71 institutions and factors associated
with the outcome like birth-weight, APGAR score,
gestational age, age at presentation and associated
cardiac anomaly was analyzed. In their study
APGAR score was found to be the most useful
predictive equation which correlated well with the
poor outcome[9].
Blood gas analysis was done on all babies soon
after birth and an initial pH < 7 was seen in seven
(70%) babies with 100% mortality. Mishalany et al
analysed 55 patients with CDH and found that
those with uncorrected pH of < 7 had 100%
mortality in their series whereas those with a pH
between 7 - 7.2 had 50% mortality. Early surgery
and correction of acidosis did not improve the
survival. They concluded that initial pH was of
great prognostic importance[10]. Initial pO2 of < 60
mmHg was seen in eight (80%) of our babies with
100% mortality and > 60 mmHg in two babies who
survived.
December 2006
Several reports documented the fact that an
initial pCO 2 of > 40 mmHg is associated with high
mortality rate (between 75-100%)[11,12,13]. The outcome of
CDH presenting in first six hours of life correlates
to the degree of pulmonary hypoplasia as indicated
by preoperative index of ventilation which if >1000
indicates a very high mortality. Ventilation index, a
ratio of mean airway pressure x respiratory rate
was < 1000 in three (30%) cases with 33.3%
mortality and > 1000 in seven (70%) cases with
100% mortality. Bohn et al observed that when
ventilation index in their series of 66 infants was >
1000 the mortality was 50%. Associated PPHN was
seen in eight (80%) babies from our series with
100% mortality. Three (30%) babies developed
pneumothorax with 100% mortality. Chou et al in
their review of 32 babies found very high mortality
rates with associated pneumothorax and PPHN.
Due to lack of facilities of hyperventilation and
ECMO in our unit all the babies were put on
conventional ventilation. Drugs like tolazoline and
prostacyclin, which are thought to reduce PPHN,
were tried in four (40%) cases with 100% mortality.
In a study by Bos et al, in 52 high risk babies with
CDH who needed ventilation within six hours with
documented PPHN in 21 (46%) cases, tolazoline
did not reduce the oxygen index or alveolar arterial
oxygen difference[14].
Out of six babies who were transferred, four
(40%) were operated upon. Two (20%) were less
than five days old and had 100% mortality while
the other two babies (20%) were more than five
days old and survived. The primary problem in
these babies is respiratory failure not due to lung
compression by the herniated viscera but due to
pulmonary hypoplasia and associated pulmonary
hypertension. Weber et al compared the survival
rates of the three eras of management of CDH on
203 neonates. In era 1 with immediate repair the
survival was 42% as compared to era 3 in which
there was delayed repair of CDH with ECMO
where the survival rate was 96%[13]. David et al
evaluated the impact of non-standard ventilatory
strategy on survival in CDH and concluded that
hyperventilation with alkalinisation had a
detrimental effect and should be abandoned and
that the survival rates of delayed surgery and
ECMO were significantly higher [15].
Ventilatory strategies that minimize airway
pressure reduce the barotrauma and lung injury to
the severely hypoplastic lungs, thereby improving
survival of babies with CDH. Gentle ventilation
which allows arterial pCO2 to be slightly higher
than normal (permissive hypercapnia) and
marginal post-ductal oxygenation are associated
with higher survival rates than conventional
ventilation. ECMO is most successful when used
December 2006
KUWAIT MEDICAL JOURNAL
for reversible pulmonary diseases like PPHN,
meconium aspiration or PFC. In diaphragmatic
hernia, ECMO has been used successfully to
prevent barotrauma from mechanical ventilation
and allow vasculature remodeling and thereby
stabilize the baby before surgical repair. Due to
underlying pulmonary hypoplasia in diaphragmatic
hernia, the gain by ECMO is not substantial as
compared to that in meconium aspiration
syndrome. Comparative data by Ann Arbor,
Michigan ECMO organization study in 1997
indicated that out of 4519 babies treated with
ECMO for meconium aspiration, 94% survived as
compared with only 54% survival out of 2627
babies treated for diaphragmatic hernia.
CONCLUSION
CDH due to its fundamental complex problems
of pulmonary hypoplasia and hypertension still
remains a management challenge with its high
mortality. As compared to other studies the
mortality rates in our study was quite high due to
non-availability of newer modes of ventilation and
ECMO and delay in stabilization and transfer of
such neonates.
REFERENCES
1.
2.
3.
Muratore CS, Wilson JM. Congenital diaphragmatic hernia:
where are we and where do we go from here? Semin
Perinatol 2000; 24: 418-428.
Juretschke LJ. Congenital diaphragmatic hernia: update
and review. J Obstet Gynecol Neonatal Nurs 2000; 30:259268.
Ruff SJ, Campbell JR, Harrison DF, et al. Pediatric
4.
5.
6.
7.
8.
9.
10.
11.
12.
13.
14.
15.
291
diaphragmatic hernia, an eleven-year experience. Am J
Surg 1980; 139:641-645.
Puri P, Gowman WA. Natural history of congenital
diaphragmatic hernia : Implications for management. J
Pediatr Surg 1984; 19:394-397.
Anderson KD. Congenital diaphragmatic hernia. In
Raviton MM. Ped Surgery, 4th ed, Chicago Year book
Publisher Inc, p 1986.
Bell MJ, Temberg JL. Antenatal diagnosis of diaphragmatic
hernia. Pediatr 1977; 60:738-742.
Fauza DO, Wilson JM. Congenital diaphragmatic hernia
and associated anomalies: their incidence, identification
and impact on prognosis. J Pediatr Surg 1994; 29:1113-1117.
Wenstorm KD. Weiner CP, Hanson J. A 5-year statewide
experience in congenital diaphragmatic hernia. Am J Obstet
Gynecol 1991; 165: 838-842.
Department of Surgery, University of Texas-Houston
Medical School : Estimating disease severity of congenital
diaphragmatic hernia in the first 5 minutes of life. The
congenital diaphragmatic hernia study group. J Pediatr Sur
2001; 36:141-145.
Mishalany HG, Nakada K, Woolley MM. Congenital
diaphragmatic hernia: eleven years experience. Arch Surg
1979; 114:1118-1123.
Chou HC, Tang JR, Lai HS, et al. Prognostic indicators of
survival of infants with congenital diaphragmatic hernia. J
Formos Med Assos 2001; 100:173-175.
Bohn D, Tamura M, Perrin D, et al. Ventilatory predictors of
pulmonary hypoplasia in congenital diaphragmatic hernia,
confirmed by morphological assessment. J Pediatr 1987;
111:423-431.
Weber TR, Kountzman B, Dillon PA, Silen ML. Improved
survival in congenital diaphragmatic hernia with evolving
therapeutic strategies. Arch Surg 1998; 133:498-502.
Bos AP, Tibboel D, Koot VC, Hazebroek FW. PPHN in high
risk congenital diaphragmatic hernia patients: incidence
and vasodilator therapy. J Pediatr Surg 1993; 28:1463-1465.
David W Kays, Maz R Langham, Danile J, et al. Detrimental
effects of standard medical therapy in congenital
diaphragmatic hernia. Ann Surg 1999; 230(3).
KUWAIT MEDICAL JOURNAL
December 2006
Original Article
Anomalous Coronary Artery from the Opposite Coronary
Sinus in Young Children
Mustafa A Al-Qbandi1, Jeffrey Smallhorn2
Department of Pediatrics and Congenital Heart Diseases, Chest Disease Hospital, Kuwait
Division of Cardiology, Department of Pediatrics, The Hospital for Sick Children and the University of Toronto, Ontario,
Canada
1
2
Kuwait Medical Journal 2006, 38 (4): 292-299
ABSTRACT
Objective: To report the management of anomalous
coronary artery (ACA) from the wrong aortic sinus and
review the literature
Background: ACA is a rare congenital lesion. It is
associated with sudden death, particularly in young
adolescents.
Design: Retrospective study (1990 - 2004)
Methods: All patients with interarterial single coronary
artery arising from the aortic sinus were studied. Seven
patients were identified. Transthoracic and transesophageal
echocardiography were performed using high frequency
transducers. Other tests used were: A 12-lead echocardiogram, 24-hour Holter, coronary angiography, exercise
and Dobutamine stress testing and single-photon
emission computed tomographic myocardial scintigraphy
(SPECT). Extracorporeal membrane oxygenation (ECMO)
was used for severe left ventricular dysfunction.
Results: There were five boys and two girls. All had an
intramural course of the coronary arteries. Their age
range was between 2 weeks to 15 years. In four out of
seven cases, it was an anomalous left coronary artery
from the right anterior aortic sinus (ALCA-RAS). The
other three cases were of an anomalous right coronary
artery from the left aortic sinus (ARCA-LAS). In one
patient, Doppler evidence of the intramural coronary
artery stenosis was documented at cardiac arrest and
ECMO support was needed.
Conclusion: As part of first echocardiography study, all
patients, regardless of their age, should have their
coronary arteries screened in the echocardiography
laboratories. Once coronary artery abnormalities are
detected (i.e., arising from opposite sinus), efforts should
be made to look for any evidence of ischemia either
through noninvasive or invasive techniques. Anomalous
left coronary origin from the right sinus of Valsalva can
result in significant myocardial ischemia and infarction.
KEYWORDS: anomalous coronary artery, echocardiography, intramural coronary artery
INTRODUCTION
The origin of one of the coronary arteries from
the wrong aortic sinus of Valsalva with a proximal
course between the aorta and pulmonary artery is a
rare congenital lesion[1-4] (Fig. 1). The incidence of
ectopic coronary origin from the aorta in the
population is unknown. Its estimates in cardiac
catheterization laboratory populations approximate
0.6%[5]. It is associated with life-threatening
conditions or sudden death, particularly in young
adolescents[6-8] where the majority of cases are
diagnosed at autopsy[4;6] [9-11]. Some authors[12] report
that this anomaly is the second most common
cause of sudden death among young athletes. The
diagnosis is usually made either after an acute
event, or more recently as an incidental finding on
routine echocardiography screening for other
forms of congenital heart disease. We report seven
cases where routine screening by echocardiography detected this anomaly and discuss potential
management implications in this group. Also, we
describe the findings in a case who presented with
a sudden cardiac event.
METHODS
From our database (n Kuwait and Canada) we
identified all cases of ALCA from the wrong aortic
sinus between1990-2004. All patients represented
incidental cases that were being evaluated for
reasons not associated with the abnormal coronary
artery. The following tests were performed:
l Echocardiography: A complete transthoracic
two-dimensional echocardiogram was performed
in each case using an Advanced Technology
Laboratory (HDI 5000) or a Hewlett Packard (HP
5500) imaging system utilizing high frequency
transducers. In three cases, transesophageal
echocardiography was utilized to obtain further
images of the abnormal coronary artery as well as
Doppler velocity profiles.
Address correspondence to:
Dr. Mustafa A. Al-Qbandi DCH, FAAP, FRCPC, Department of Pediatric and Congenital Heart Diseases, Chest Disease Hospital, P.O.BOX:
4082, Safat, 13081, Kuwait. Tel: +965- 4829613, Fax: +965- 4829613, E-mail: [email protected]
December 2006
KUWAIT MEDICAL JOURNAL
293
Table 1: Summary of the cases of ACA
Case Age
Sex
Diagnosis
Symptoms
12-Lead
ECG
EchoCardiography
Angio- DSE
graphy
Myocardial Outcome
Perfusion
scan
1
2
2-weeks
4 years
M
F
ALCA-RAS
ALCA-RAS
Murmur
Cardiac arrest
TTE
TTE&TEE
No
No
No
No
No
No
3
4
10 years
14 years
M
M
ALCA-RAS
ALCA-RAS
TTE&TEE
TTE
Yes
Yes
Yes
No
Yes
Yes
Alive
Death
post surgery
Alive
Alive
5
6
7
15 years
8 years
2-weeks
M
M
F
ARCA-LAS
ARCA-LAS
ARCA-LAS
Murmur
Pre-renal transplant
assessment
Near syncope
Murmur
Murmur
Normal
Severe ST-depression&
Left anterior hemi block
Normal
Normal
Normal
Normal
Normal
TTE&TEE
TTE
TTE
Yes
No
No
Yes
No
No
No
No
No
Alive
Alive
Alive
ALCA-RAS = anomalous left coronary artery from right aortic sinus, ARCA-LAS = anomalous right coronary artery from the left aortic sinus
DSE = dobutamine stress echocardiography, F = female, M = male, TEE = transesophageal echocardiography, TTE = transthoracic echocardiography
l 12-lead ECG: All patients had a resting
electrocardiogram (ECG).
l 24-hour Holter: A Holter monitor was
performed in four cases.
l Exercise testing: An exercise stress test was
done in two cases.
l Coronary angiography: In three cases,
selective coronary artery angiograms were done.
l Dobutamine stress test: This was done in two
cases.
l Single-photon emission computed tomographic
myocardial scintigraphy (SPECT): Performed with
intravenous administration of 99mTc-Sestamibi
during exercise and at rest 24 hours later in two
cases.
Extracorporeal membrane oxygenation (ECMO)
was used in one patient for severe left ventricular
dysfunction presenting with evidence of myocardial
infarction and life threatening arrhythmia leading
to cardiac arrest.
RESULTS
Presentation and clinical features
Seven patients were identified (Table 1). Their
ages ranged between two weeks to 15 years
(median = 10 years) and there were five males and
two females. Anomalous left main coronary artery
from the right aortic sinus was identified in four
cases and anomalous right coronary from the left
sinus in three. There was only one death (case 2)
during the course of the study.
In four cases, the reason for referral was a
cardiac murmur, in one it was for evaluation of a
patent ductus arteriosus in a neonate with
subsequent surgical ligation (case 1). An episode of
near syncope was the reason for referral (case 6),
which was initially felt to be vasovagal. This patient
had no complaints of chest pain or palpitations. In
case 4 the patient had the abnormality detected as
part of a pre-renal transplant assessment in a case
with nephrosclerosis. The last patient (case 2) had a
Fig. 1: Coronary artery sketch: Fig.1-1: Normal coronary artery anatomy
where the left coronary artery arises from the left aortic sinus and the
right coronary artery arises from the right coronary sinus (appropriate
sinuses). Fig. 1-2: Origin of the right coronary artery from the left aortic
sinus. Fig. 1-3: Anomalous left coronary artery from the right aortic sinus.
Notice the abnormal course and compression of the segment of the
coronary artery between the aorta and the pulmonary artery
(inappropriate sinuses). Ao = Aorta, PA= Pulmonary artery, L=Left,
R=Right, N=non-coronary cusp, LAD=Left anterior descending, Cx=
Circumflex artery, RCA= Right coronary artery.
sudden cardiac event outside our institution where
the diagnosis was made by an outside pediatric
cardiologist in the emergency room. The patient
was subsequently transferred to our intensive care
unit for further management and required ECMO
support for low cardiac output.
All patients were not related to one ethnic
group. Incidentally, all patients who were referred
for evaluation of a cardiac murmur turned out to
have an innocent murmur. Parents reported no
similar problem in their close families. All patients
had no birth defects. Only one patient (case 1) had
PDA ligation and no other associated cardiac
defects were detected in others. To date, none of the
patients on follow up required surgery, except for
the deceased one (case 2).
Electrocardiograms (ECG’s) and exercise tests: All
were normal at presentation except in case 2, which
demonstrated severe ST-segment depression in all
the precordial and inferior leads with evidence of
left anterior hemi-block. All recorded 24-hour
Holter monitors and exercise tests were normal.
Echocardiography: All patients were diagnosed
initially by transthoracic echocardiography (Table 1
and 2). In three cases transesophageal echocardio-
294
Anomalous Coronary Artery from the Opposite Coronary Sinus in Young Children
Fig. 2: (A) Parasternal long axis view through the aortic root in a boy with
anomalous left main coronary artery (LMCA) with an intramural segment
of the LMCA giving the double border appearance of the aortic wall
(arrowhead). Seen is a single ostium with an origin from the right
coronary cusp. Right coronary artery=RCA, aorta=Ao, left ventricle=LV,
right ventricle=RV.
Table 2: Summary of echocardiographic features
Parameter
ALCA-RAS
ARCA-LAS
Origin
Ostium
Orifice (3D-image)
Intramural
Proximity to commissure
2D image:
Parasternal long axis
RAS
Mostly large single
Rounded or slit-like
Segment course long interarterial
close
LAS
Usually two separate
Mostly slit-like
Short interarterial
Very close
Parasternal short axis
Doppler color flow
Spectral Doppler flow
Double border appearance
of aortic wall
Take off at 10 o’clock
at 110 degrees followed by
acute angle LMCAtake off
(hockey-stick appearance)
Aliasing usually seen before
LMCAbifurcation
Usually low pandiastolic &
Slightly increased systolic flow
No
Take off at 12 or 1 o’clock
at 160 degrees
December 2006
Fig. 2:(B) Parasternal short axis view showing the intramural segment of
part of the long course of the left main coronary artery (arrowheads).
Aorta=Ao, pulmonary artery=PA.
intramural segment was clearly seen in all cases.
In those patients with anomalous right coronary
artery from the left aortic sinus, the parasternal
long axis view did not show the double border
appearance of the aortic wall. The parasternal short
axis view revealed the slit like orifice of the
anomalous right coronary artery, which was even
more clearly demonstrated by transesophageal and
three-dimensional echocardiography (Fig. 3 A & B).
In both cases the orifice was very close to the
commissure between the right and left sinuses
which was in contrast to cases with anomalous
origin of the left coronary artery from the right
aortic sinus.
(spear-like appearance)
No
Normal flow pattern
ALCA-RAS= Anomalous left coronary artery from right aortic sinus
ARCA-LAS= Anomalous right coronary artery from left aortic sinus
LMCA= left main coronary artery
graphy was performed to further delineate the
anatomy including a 3-dimensional reconstruction in
case 1.
In those patients with anomalous left coronary
artery from the right aortic sinus the parasternal
long axis view demonstrated the large single
ostium, which then bifurcated into right and left
main coronary arteries. The left main coronary
artery then ran between the aorta and pulmonary
artery with an intramural segment within the aortic
wall resulting in a double border appearance of the
anterior aortic wall (Fig. 2A). Similarly, the parasternal
short axis view demonstrated a single large ostium
that arose from the right anterior aortic sinus,
which then bifurcated, into right coronary artery
and a long interarterial / intramural segment (Fig.
2B). In all cases the left main coronary artery
formed an acute angle with its origin. The
Doppler flow patterns:
Two spectral Doppler flow characteristics were
identified. Firstly, in those with no evidence of
obstruction the appearance was that of low velocity
diastolic flow with a short but slightly increased
systolic flow velocity. This appearance correlated
with mild color aliasing seen in the intramural
segment of the left main coronary just proximal to
its bifurcation (Fig. 4 A & B). In the case with a
cardiac event there was clear evidence of an
obstructive flow pattern in the intramural segment,
with laminar flow in the proximal interarterial
segment. Of interest, this was only seen on the
transesophageal study, as the intramural segment
of the left coronary artery was stenotic and difficult
to image from the transthoracic location. As the left
main coronary artery exited from its intramural
course, the vessel and its proximal branches
became dilated with evidence of re-laminization of
the Doppler flow signal. Spectral Doppler flow
showed a high velocity systolic and diastolic flow
pattern in the intramural segment with the former
being 40 cm/sec and the latter 180 cm/sec. Of note,
the spectral pattern at the site of origin of the left
coronary artery and in the dilated segments
December 2006
KUWAIT MEDICAL JOURNAL
295
Fig. 3: (A) Transesophageal echocardiographic image at mid-esophagus in
short axis view at the level of aortic sinuses showing the three sinuses and
the origin of the right coronary artery (RCA) from the left aortic sinus.
Note the proximity to the anterior commissure.
Fig. 3: (B) Three-dimensional image of the coronary artery ostia in a case
of ARCA-LAS. This shows the slit-like orifice of the anomalous right
coronary artery and rounded orifice of the left main coronary artery, both
originating from the left coronary sinus.
Fig. 4: (A) A normal spectral Doppler flow pattern seen in the anomalous
left main coronary artery. A pandiastolic (D) and a short systolic (S) flow
are seen. This shows a non-obstructed flow pattern.
demonstrated a lower velocity pattern. (Fig. 5 A& B).
M-Mode: All patients (except case 2) had normal
cardiac systolic and diastolic functions at first study
and on follow up. All cardiac chamber dimensions
were also normal. In case 2, the patient presented
with severe left ventricular dysfunction and wall
motion abnormalities of the anterolateral wall. Her
left ventricular ejection fraction was 5-10%
requiring ECMO support.
Angiography: Three cases (3, 4, and 5) underwent
selective coronary angiography. The angiographic
pictures correlated well with echocardiographic
images and did not add any additional information
(Fig. 6).
Dobutamine stress echocardiography (DSE): Two
cases (3 & 5) underwent this type of study to look
for any evidence of wall motion abnormalities or
ischemic changes. In case 3, the DSE was
interpreted as demonstrating mild hypokinesia
involving the apical anterior wall and the mid
anterior septum. With an increasing dose of
Fig. 4: (B) Doppler color flow mapping in the same patient, which shows
very slight color aliasing of the intramural segment of the left main
coronary artery (LMCA).
Dobutamine, there was progressive increase in
contractility involving all segments, apart from
those mentioned above which remained mildly
hypokinetic, though improved compared to
baseline. This was interpreted as consistent with
prior myocardial damage. In case 5, the study was
interpreted as being normal.
Myocardial perfusions scan: In two cases (3 & 4)
single-photon emission computed tomographic
myocardial scintigraphy (SPECT) was performed
with intravenous administration of 99mTc-Sestamibi
during exercise and at rest 24 hour later. Both
showed no evidence of perfusion defects.
296
Anomalous Coronary Artery from the Opposite Coronary Sinus in Young Children
Fig. 5: (A) In comparison to the case in Fig. 3, severe stenosis of the
interarterial, intramural segment of the left main coronary artery before
its bifurcation in a patient who presented in cardiac arrest. The
transesophageal Doppler color flow pattern showing color aliasing at the
stenotic intramural segment.
December 2006
Fig. 5: (B) Spectral Doppler flow wave showed high peak diastolic and
systolic velocities, which did not change with intravenous injection of
nitroglycerine.
Fig. 7: Histology specimen showing the severe fibrointimal proliferation of
the intramural segment resulting in severe stenosis.
Fig. 6: Right anterior oblique projection of the single coronary
angiograms. This shows an unusually long segment of the left main
coronary artery initially coursing posteriorly.
Surgery: Only one patient underwent surgery (case
2). After a brief period of stabilization on ECMO for
severe left ventricular dysfunction, the patient
underwent surgical reimplantation of the
anomalous left coronary artery. A vertical incision
was made in the distal non- intramural segment of
the left coronary artery (LCA) proper, which
appeared thin-walled and measured 2-3 mm in
diameter. A direct tissue connection was made
between the inferior apex of the vertical aortic
incision and the corresponding incision in the LCA.
The anterior aspect of the connection between the
LCA and the ascending aorta was augmented with
a triangle-shaped patch of autologous pericardium.
The segment of LCAbetween the origin of the LCA
and the reconstructed LCA was not interrupted
surgically with the LCA reimplantation. This
patient died within 48 hours of surgical repair. The
autopsy revealed severe and diffuse left ventricular
myocardial infarction and a single coronary artery
that arose from the right anterior sinus. The left
main coronary artery was intramural in its course
and showed stenosis at the segment just prior to
LMCA bifurcation. The new LMCA ostium was
narrowed at its suture line. Histological section of
the narrowed intramural segment showed evidence
of severe fibrointimal proliferation (Fig. 7).
DISCUSSION
When the left coronary artery arises from the
right sinus of Valsalva and courses between the
aorta and pulmonary artery, it invariably assumes
an intramural course as it enters the aortic wall at
an acute angle with typical flattening of the
lumen[6;13;14]. This anomaly has strong predominance
in males with rare occurrences in females. Patients
often have a slit-like orifice of the LMCA origin or
valve-like ridges at the ostium[4,6,10]. The angiographic
December 2006
KUWAIT MEDICAL JOURNAL
findings demonstrate an end-on origin of the
LMCA followed by a posterior, cranial, and
leftward course[3,15,16]. Dynamic systolic compression
of the intramural portion of the LMCA has been
observed during angiography and may potentially
contribute to periods of ischemia.
Taylor et al[11,17], reported that younger patients
(less than or equal to 30 years of age) with an
isolated coronary artery anomaly are at risk of
dying suddenly and with exercise. The association
of this anomaly with exercise-related sudden death
has been explained by three factors[14,18]: Firstly, an
outward expansion of the roots of both the aorta
and pulmonary trunk during exertion, which can
cause further compression of the ostial lumen of the
anomalous artery; Secondly, the anomalous vessel
can be compressed against the root of the
pulmonary trunk, where it is firmly anchored to the
infundibular septum, when the pulmonary trunk
and the aortic root dilate during exertion; Thirdly,
myocardial oxygen requirements increase with
exertion and the consequence of myocardial
ischemia may trigger life threatening ventricular
arrhythmia and sudden death.
Jureidini and associates[9,19] reported color
Doppler mapping of the anomalous course of the
LMCA between the aorta and pulmonary artery in
a child. In our series, it is clearly demonstrated that
a careful echocardiographic search for coronary
anomalies can aid in their detection. Indeed the
routine in our laboratory is to evaluate the coronary
arteries in all new cases. If the anomaly is suspected
and transthoracic echocardiographic images are not
clear, then transesophageal echocardiography
should be performed after the patient is
stabilized[20]. Simply, identifying a coronary artery
between the two arterial roots does not necessarily
imply an intramural segment [21]. Although we
maintain that angiography remains the current
“gold standard’’, magnetic resonance imaging
(MRI) and ultrafast computed tomography may be
useful adjunctive tests. MRI showed a
complimentary role and appears a promising tool
for identifying such anomalies [18,22]. Recently,
intravascular ultrasound and pressure-wire
methods have been used for sub-classifying
anomalous coronary arteries from opposite sinus
and other coronary anomalies[14].
The role of stress evaluation as a predictor of
ischemia in these cases when detected as an
incidental finding is unclear. Although we have
been using dobutamine as our agent of choice in
pediatric patients, adenosine, arbutamine or
dipyridamole are other agents used frequently in
adult patients[13,23,24]. There is, however, enough data
to support Dobutamine stress test in patients with
Kawasaki disease[25]. In case 2, it was recommended
297
to the family that PET (positron emission
tomography) might be useful adjunct as this has the
added advantage of assessing both flow and
metabolic activity[26].
While the diagnosis of this lesion has been
facilitated by careful echocardiographic evaluation
of the coronary arteries [27], the indication for
intervention is less clear. The use of extracorporeal
membrane oxygenation (ECMO) is justified in
certain cases with severely reduced ventricular
systolic function as a bridge to heart
transplantation[28]. Certainly, in those with evidence
of ischemia the need for surgical intervention is
fairly clear. However, in pediatric patients where
the finding is incidental, with no evidence of
ischemia at rest or on stress, the argument for
intervention is less compelling. This relates to the
lack of long term data in those young patients who
have undergone surgery, versus the natural history
in a case where the finding is incidental. Although
there are multiple case reports of the relationship
between this lesion and ischemia, there are no
studies that address the frequency of ischemia in
asymptomatic patients. There is medium term data
in complete transposition of great arteries and an
intramural left coronary artery [29]. Although an
arterial switch is the current treatment of choice,
postoperative ischemia is far more prevalent than
cases with the more usual coronary artery
patterns[30,31]. One could argue that there are
younger patients than the majority of cases
identified with an intramural left coronary artery,
however, a comparison of the natural history
versus treated population are absent.
The operative repair is the one described by
Mustafa and colleagues[13,32] in which the intramural
segment of the LMCAis unroofed after detachment
of the intercoronary commissure, with creation of a
neocoronary ostium in the left sinus of Valsalva.
Subsequently, the intercoronary commissure is resuspended. In adult population, the incidence of
late cardiac events (late cardiac death, re-operation,
myocardial infarction) was lower in patients who
received internal thoracic artery graft versus
saphenous vein graft and had better survival rate at
eight years (91.1% versus 85.3%, respectively)[33]. In
contrast, long-term patency and re-operation rates
have yet to be determined in the pediatric
population. On the basis of a literature review and
their own experience with this lesion, Liberthson et
al[5] have found that the average age of the 20
reported patients who died suddenly was 16 years
(range 1 - 36 years). All of their six older patients
(age 36 to 70 years) with this anomaly had angina
pectoris and atherosclerotic vessels. This difference
may relate to the more rigid coronary arteries in an
older individual being less susceptible to torsion
298
Anomalous Coronary Artery from the Opposite Coronary Sinus in Young Children
and resultant ischemia in comparison to a young
adolescent male. He also found that atrial pacing
may reveal ischemic changes during cardiac
catheterization. This has lead some cardiologist to
use calcium channel blocking agent or beta-blocker
to limit the attainment of threateningly high heart
rates. In general, management is guided by: mode
of presentation, age at presentation, size of ectopic
coronary artery, presence of related proximal
coronary artery obstruction, and lifestyle of
individual patient. Patients younger than 40 years
with large ectopic arteries, functional and anatomic
compromise, and ischemic or arrhythmic complications
require intervention. For patients older than 50
years, specific therapy are rarely required. Lastly,
for patients between 40 and 50 years care must be
individualized[34].
Our present recommendation is the following;
as part of first echocardiography study, all patients,
regardless of their age, should have their coronary
arteries screened in the echocardiography
laboratories. Once coronary abnormalities are
detected (i.e., origin from the opposite sinus),
efforts should be made to look for any evidence of
ischemia either through invasive or noninvasive
techniques. Anomalous left coronary origin from
the right sinus of Valsalva can result in significant
myocardial ischemia and infarction.
REFERENCES
1.
2.
3.
4.
5.
6.
7.
8.
9.
Basso C, Maron BJ, Corrado D, Thiene G. Clinical profile of
congenital coronary artery anomalies with origin from the
wrong aortic sinus leading to sudden death in young
competitive athletes. J Am Coll Cardiol 2000; 35:1493-1501.
Chaitman BR, Lesperance J, Saltiel J, Bourassa MG. Clinical,
angiographic, and hemodynamic findings in patients with
anomalous origin of the coronary arteries. Circulation 1976;
53:122-131.
Kimbiris D. Anomalous origin of the left main coronary
artery from the right sinus of Valsalva. Am J Cardiol 1985;
55:765-769.
Lipsett J, Cohle SD, Berry PJ, Russell G, Byard RW.
Anomalous coronary arteries: a multicenter pediatric
autopsy study. Pediatr Pathol 1994; 14:287-300.
Liberthson RR, Dinsmore RE, Fallon JT. Aberrant coronary
artery origin from the aorta. Report of 18 patients, review of
literature and delineation of natural history and
management. Circulation 1979; 59:748-754.
Cheitlin MD, De Castro CM, McAllister HA. Sudden death
as a complication of anomalous left coronary origin from
the anterior sinus of Valsalva, A not-so-minor congenital
anomaly. Circulation 1974; 50:780-787.
Daehnert I, Rotzsch C, Krause S, Dorszewski A, Kostelka M.
Syncope in a child owing to intramural course of the left
coronary artery. Acta Paediatr 2003; 92:1339-1342.
Massih TA, Clur SA, Bonhoeffer P. Exertional pulmonary
edema revealing anomalous origin of the left coronary
artery from the right coronary aortic sinus. Cardiol Young
2002; 12:78-80.
Jureidini SB, Eaton C, Williams J, Nouri S, Appleton RS.
Transthoracic two-dimensional and color flow echocardiographic diagnosis of aberrant left coronary artery. Am Heart
December 2006
J 1994; 127:438-440.
10. Kragel AH, Roberts WC. Anomalous origin of either the
right or left main coronary artery from the aorta with
subsequent coursing between aorta and pulmonary trunk:
analysis of 32 necropsy cases. Am J Cardiol 1988; 62:771777.
11. Taylor AJ, Rogan KM, Virmani R. Sudden cardiac death
associated with isolated congenital coronary artery
anomalies. J Am Coll Cardiol 1992; 20:640-647.
12. Maron BJ, Wolfson JK, Epstein SE, Roberts WC. Intramural
(“small vessel”) coronary artery disease in hypertrophic
cardiomyopathy. J Am Coll Cardiol 1986; 8:545-557.
13. Mustafa I, Gula G, Radley-Smith R, Durrer S, Yacoub M.
Anomalous origin of the left coronary artery from the
anterior aortic sinus: a potential cause of sudden death.
Anatomic characterization and surgical treatment. J Thorac
Cardiovasc Surg 1981; 82:297-300.
14. Angelini P, Velasco JA, Ott D, Khoshnevis GR. Anomalous
coronary artery arising from the opposite sinus: descriptive
features and pathophysiologic mechanisms, as documented
by intravascular ultrasonography. J Invasive Cardiol 2003;
15:507-514.
15. Ishikawa T, Brandt PW. Anomalous origin of the left main
coronary artery from the right anterior aortic sinus:
angiographic definition of anomalous course. Am J Cardiol
1985; 55:770-776.
16. Rigatelli G, Docali G, Rossi P, et al. Congenital coronary
artery anomalies angiographic classification revisited. Int J
Cardiovasc Imaging 2003; 19:361-366.
17. Taylor AJ, Byers JP, Cheitlin MD, Virmani R. Anomalous
right or left coronary artery from the contralateral coronary
sinus: “high-risk” abnormalities in the initial coronary
artery course and heterogeneous clinical outcomes. Am
Heart J 1997; 133:428-435.
18. Zeppilli P, dello RA, Santini C, et al. In vivo detection of
coronary artery anomalies in asymptomatic athletes by
echocardiographic screening. Chest 1998; 114:89-93.
19. Frommelt PC, Frommelt MA, Tweddell JS, Jaquiss RD.
Prospective echocardiographic diagnosis and surgical
repair of anomalous origin of a coronary artery from the
opposite sinus with an interarterial course. J Am Coll
Cardiol 2003; 42:148-154.
20. Salloum JA, Thomas D, Evans J. Transoesophageal
echocardiography in diagnosis of aberrant coronary artery.
Int J Cardiol 1991; 32:106-108.
21. Pasquini L, Parness IA, Colan SD, Wernovsky G, Mayer JE,
Sanders SP. Diagnosis of intramural coronary artery in
transposition of the great arteries using two-dimensional
echocardiography. Circulation 1993; 88:1136-1141.
22. Phoon CK, Van SJ, Moore PA, Brook MM, Haas GS, Higgins
CB. Aberrant left coronary artery arising from the right
sinus of Valsalva with a right coronary arteriovenous
malformation. Pediatr Cardiol 1997; 18:385-388.
23. Moodie DS, Gill C, Loop FD, Sheldon WC. Anomalous left
main coronary artery originating from the right sinus of
Valsalva: Pathophysiology, angiographic definition, and
surgical approaches. J Thorac Cardiovasc Surg 1980; 80:198205.
24. Kimball TR, Witt SA, Daniels SR. Dobutamine stress
echocardiography in the assessment of suspected
myocardial ischemia in children and young adults. Am J
Cardiol 1997; 79:380-384.
25. Zilberman MV, Goya G, Witt SA, Glascock B, Kimball TR.
Dobutamine stress echocardiography in the evaluation of
young patients with Kawasaki disease. Pediatr Cardiol
2003; 24:338-343.
26. Cooper RS, Singh S, Robenson W, Chaly T, Margouleff,
Lacorte MA. Pediatric Cardiac PET Imaging. Progress in
December 2006
KUWAIT MEDICAL JOURNAL
Pediatric Cardiology 1997; 7:131-139.
27. Jureidini SB, Marino CJ, Singh GK. Congenital Coronary
Artery Abnormalities in Children. 2001; 3:393-401.
28. Reich JD, Sutherland J, Winn K, Pettignano R. Intramural
anomalous left coronary artery from the right sinus of
Valsalva supported with venoarterial extracorporeal
membrane oxygenation. South Med J 1999; 92:714-716.
29. Asou T, Karl TR, Pawade A, Mee RB. Arterial switch:
translocation of the intramural coronary artery. Ann.Thorac
Surg 1994; 57:461-465.
30. Vogel M, Smallhorn JF, Gilday D, et al. Assessment of
myocardial perfusion in patients after the arterial switch
operation. J Nucl Med 1991; 32:237-241.
31. Dae MW. Myocardial perfusion after repair of
299
transposition: is it worth the switch? J Am Coll Cardiol
1994; 24:778-779.
32. Romp RL, Herlong JR, Landolfo CK, et al. Outcome of
unroofing procedure for repair of anomalous aortic origin
of left or right coronary artery. Ann Thorac Surg 2003;
76:589-595.
33. Kawachi K, Kitamura S, Morita R, et al. Late results of
coronary artery bypass grafting with the internal thoracic
artery. Kyobu Geka 1992; 45:665-670.
34. Michael A. Gatzoulis, Gary D. Webb, Piers E.F. Daubeney.
Congenital Anomalies of the Coronary arteries. In: Michael
A.Gatzoulis, Gary D. Webb, Piers E.F. Daubeney, editors.
Diagnosis and Management of Adult Congenital Heart
Disease, Elsevier; 2003, p 425-431.
KUWAIT MEDICAL JOURNAL
December 2006
Original Article
Results of Combined Proximal Crescentic Metatarsal
Osteotomy and Modified Distal Soft Tissue Procedure in
Severe Hallux Valgus
Ibrahim MAAl-Kussary1,2, Fathy Khallaf 1, Mahmoud El Rayes 1, Mustafa Al Akkad1
Department of Orthopedics, 1Al-Jahra Hospital, 2Al-Razi Hospital, Kuwait
Kuwait Medical Journal 2006, 38 (4): 300-307
ABSTRACT
Objective: To review subjective, objective, and
complication results of surgery of combined proximal
crescentic metatarsal osteotomy and modified distal soft
tissue procedure in adult foot severe hallux valgus
deformities
Design: Retrospective clinical study
Setting: Al-Jahra Hospital Orthopedic Department and
Al-Razi Orthopedic Hospital
Methods: We retrospectively studied the results for
thirty consecutive patients (38 feet), in whom a severe
hallux valgus deformity with hallux valgus angle (HVA)
> 40º and first / second inter-metatarsal angle (1/2 IMA)
> 16º had been corrected surgically. The surgery included
proximal crescentic osteotomy of the first metatarsal,
lateral release of the distal soft tissues, excision of the
medial eminence, plication of the medial part of the
capsule of the 1st metatarso-phalageal joint (1st MTP)
and a modification of Z-plasty lengthening of the
extensor hallucis longus (EHL) tendon. The patients
were followed up for an average of twenty-eight months
(range 17-47 months).
Results: The preoperative HVA averaged 48º and
postoperative angle averaged 13º. The preoperative 1/2
IMA averaged 18º and postoperative angle averaged 7º.
Ninety-three percent of the patients were satisfied with
the results of the procedure. They stated that, given the
same circumstances, they would have the operation
again. A clinical and radiological excellent to good
correction was achieved in 95% of the feet (excellent in
79% and good in 16%) with an average American
Orthopedic Foot and Ankle Society (AOFAS) hallux score
of 92 out of 100 points.
Complication: included recurrence of gross hallux valgus
deformity in two dissatisfied patients (2 feet, 6.6%) and
mild under-correction of six feet in four patients (13%).
However, the patients were satisfied with the relief of
pain and the cosmetic appearance of their feet.
Hypothesia along the medial aspect of the great toe
occurred in two patients (2 feet, 6.6%). Pin track infection
occurred in two patients (2 feet, 6.6%) and deep infection
in one patient. All were cured after debridment and
antibiotics.
Conclusion: According to the results of this report and
other studies in the literature, proximal crescentic
metatarsal osteotomy combined with distal lateral
release, medial repair and lengthening of the EHLtendon
is a reliable and successful surgery for treating severe
hallux valgus deformity.
KEYWORDS: hallux valgus, metatarsal deformity, proximal crescentic osteotomy
INTRODUCTION
The deformity of hallux valgus is the lateral
deviation of the great toe. It is associated with other
pathological features which include: medial
deviation of the first metatarsal (metatarsus primus
varus) with increased inter-metatarsal angle (IMA)
between the first and second metatarsals,
prominent medial eminence, contracted soft-tissue
structures on the lateral side of the great toe, lateral
displacement of the sesamoids and contracture of
the extensor and flexor tendons leading to lateral
rotation of the metatarsal head and pronation of the
hallux[1-4]. A hallux valgus angle (HVA) > 40º and
inter-metatarsal angle (1/2 IMA) > 16º are the
radiological features defining severe hallux valgus.
Commonly, the severe hallux valgus is
characterized by progressive subluxation and
incongruity of the first metatarso-phalangeal joint
with altered distal metatarsal articular angle
(DMAA). The deformity is attributed to congenital
hereditary metatarsus primus varus with 55-60%
positive family history and to the acquired splayed
foot secondary to weak intrinsics with contribution
from the effect of shoe wearing [5, 6].
More than 130 different surgical procedures
have been described to treat this deformity[5,8,9]. The
main procedures to surgically treat severe hallux
valgus include: proximal osteotomy to correct the
first metatarsal deformity by opening a wedge,
closing a wedge, crescentic and proximal chevron
Address correspondence to:
Dr. Ibrahim M.A Al-Kussary, MD, Orthopedic Department, Al-Jahra Hospital, P.O. Box 723, 01009 Kuwait. Tel : (+965) 7432347, (+965)
6541933, Fax: (+965) 4588408, E-mail: [email protected]
December 2006
KUWAIT MEDICAL JOURNAL
Sammarco osteotomies with distal soft-tissue
release and medial plication. It also includes scarf,
Mau and Ludloff ostotomies[2,3,5,7,8]. The first tarsometatarsal arthrodesis is also an option in the
surgical management of severe hallux valgus with
hypermobile first ray or as salvage after failed other
bunion repair surgeries[7,9].
Post-surgical complications are always the
concern of both patients and surgeons and include:
recurrence of deformity, poor cosmetic appearance,
under-correction, over-correction with hallux varus
deformity, shortening of the first ray, and elevation
of the first ray causing transfer lesion to second
metatarsal head (transfer metatarsalgia)[3,5,8,9].
In this report, we present the subjective,
objective, radiological and complication results of
surgical treatment of severe hallux valgus by
proximal dome osteotomy with distal soft tissue
release and medial plication. We added a
modification of Z-plasty of the extensor hallux
longus (EHL) tendon through the dorso-medial
incision to the distal soft tissue procedure[11].
PATIENTS AND METHODS
Between May 1996 and April 2003, thirty
consecutive patients with thirty-eight feet of severe
hallux valgus were treated surgically in Al-Razi
Orthopedic Hospital and Jahra General Hospital,
Kuwait. The patients who were retrospectively
interviewed, gave their informed consent before
entering the trial and were examined clinically,
radiologically and complicationwise as also for
assessment of their satisfaction with the results of
the surgery. The pre and post-operative clinical
data were gathered according to guidelines
recommended by the American Orthopedic Foot
and Ankle Society AOFAS)[8]. The weight-bearing
dorso-plantar and lateral feet radiograms were
collected from the patient’s medical records and
compared with final follow-up evaluation.
Outcome:
The primary outcome of this study was the
clinical and radiological correction of the severe
hallux valgus deformity. The secondary outcome
was the patient’s satisfaction regarding the
correction of the deformity.
Clinical assessment:
The series of patient in this study included thirty
consecutive patients with thirty-eight feet, who had
a severe degree of hallux valgus deformity. The
deformity was unilateral in twenty-two patients
(73%) and bilateral in eight patients (27%) with
ratio 3:1. There were 25 female (83%) and five male
patients (17%) with ratio 5:1. The average age was
thirty-eight years and the range was 22-48 years.
301
The indication was pain and deformity in twentyseven patients (90%) including the twenty-five
females and only pain in the remaining three males
(10%). Twenty patients (67%) suffered from
problems with shoe fitting and desired operative
correction. Pre and post-operative assessment was
made according to the protocol of the American
Orthopedic Foot and Ankle Society (AOFAS). This
system provides a score ranging from Zero to 100
points, which takes into consideration both
subjective and objective elements such as pain
(maximum score = 40 points), functional capacity
(maximum score = 45 points), and hallux alignment
(maximum score = 15 points). Other factors that
were evaluated in the clinical assessment were any
limitation of daily and/or sports or recreational
activity, the type of shoes that the patient could
wear, the stability of the 1st MTP and
interphalangeal joints, and the presence of calluses.
The patient’s satisfaction with the outcome
(satisfied or unsatisfied) was also elicited. The
active and passive range of motion of the first
metatarsophalangeal joint was measured with a
goniometer (with the patient not bearing weight,
with measurement of angle between the proximal
segment of the great toe and the plantar surface of
the foot). The advantage of using the plantar surface
of the foot as the point of reference is that Zero
degree represents the functionally neutral position
of the toe. Active and passive dorsiflexion and
plantar flexion were recorded from this neutral axis
of reference. Rotational mal-alignment (pronationsupination deformity) of the great toe was graded:
no rotation was considered to be grade Zero;
rotation of less than 25 degrees, grade 1; rotation of
25 to 45 degrees, grade 2; and rotation more than 45
degrees, grade 3. The assessment was made with
the patient standing. The pronation of the hallux
was documented in the patients’ medical records in
24 patients (80%), 27 feet (71%). The hypermobility
of the metatarsocuniform (MTC) joint was not
documented in any patient’s record in this series.
Radiological assessment:
The radiological assessment of patients’ preoperative radiographs included: the HVA, the 1/2
IMA, the DMAA, the subluxation of the first
metatarso-phalangeal joint (1st MTP), the position
of the sesamoids, the lengths of the first and second
metatarsals (so that any post-operative shortening
could be measured accurately), and the osteoarthritic
changes of the metatarso-phalangeal joints.
The hallux valgus angle (HVA) is subtended by
lines along the long axis of the first metatarsal and
the proximal phalanx. Normally, the HVA is < 15º.
The inter-metatarsal angle 1/2 IMA is subtended
by lines along the longitudinal axis of the first and
302
Results of Combined Proximal Crescentic Metatarsal Osteotomy and Modified Distal Soft ..... December 2006
Table 1: Pre-operative clinical assessment
Parameter
Patient’s complaints
Pain only
Pain and deformity
Wearing shoes problems
Objective findings
Severe hallux valgus
Pronation of the hallux
Hypermobility of MTC joint
Result
n (%)
03 (10)
27 (90)
20 (67)
38 (100)
24 (63)
None
centrally in 20 feet (52.5%) and laterally in 18 feet
(47.5%). Osteoarthritis of the 1st MTP was not
observed in any of the preoperative radiographs. A
summary of the pre-operative clinical assessment is
shown in Table 1.
Fig. 1: Measurement of the DMAA (it is the angle subtended by a line
drawn perpendicular to the metatarsal articular surface and the
longitudinal axis of the first metatarsal).
second metatarsals. Normally the 1/2 IMA is < 9º.
The distal metatarsal articular angle (DMAA)
describes the lateral scope of the articular surface in
relation to the long axis of the first MT as shown in
Fig. 1. Normally, the DMAAis < 100º. The position
of the tibial sesamoid on the antero-posterior
(dorsi-plantar) radiographs was described as
medial, lateral, or central in relation to a line drawn
along the centre of the longitudinal axis of the first
metatarsal. The sesamoid was considered to be
medial, if 75 per cent of it was located medial to the
central line and as lateral, if 75 per cent of it was
located lateral to the central line. Otherwise, the
sesamoid was considered to be located centrally.
Normally, on the dorso-plantar view the metatarsal
head overlies both the tibial and fibular sesamoids
and the tibial one is medial to the longitudinal axis
of the first metatarsal.
The average pre-operative HVA was 48º (range
= 43º- 54º) and the average of pre-operative 1/2
IMA was 18º (range = 16º-22º). The MTP joint was
subluxated pre-operatively in all patients (100%),
but DMAA was normal in 13 feet (33%). The
average of the abnormal DMAA was 113º (range =
104º-117º). The tibial sesamoid was located
Statistical Analysis :
Due to the small sample size of thirty patients
(thirty-eight feet) of hallux valgus in the study,
Student - t test was chosen to estimate the significance
of the difference in pre-operative and postoperative HVA and 1/2 IMA values. Because the
outcome of the surgery was uncertain in reducing
the HVA and 1/2 IMA, an independent parametric
two- sided (tailed) test was used. This particular
kind of statistical tests allows larger variance and
have longer tails than the standard normal
distribution, which fits the data and the nature of
this study and being parametric makes it more
powerful in detecting significance. The over-all
level of alpha significance (p-value) in the study
was 0.05 and there is a 26 percent chance of at least
one spuriously significant difference over-all (p = 1[1-0.05]).
Surgical Technique:
A prophylactic antibiotic (1 gm) from the third
generation of cephalosporins is routinely injected
IV with induction of anesthesia and before application
of the tourniquet. The distal soft tissue procedure to
correct a hallux valgus deformity consists of several
steps and was performed through two incisions.
The first is made dorsally in the line of the first web
space of the foot to release the adductor hallucis,
and to release tendon from the base of the proximal
phalanx and the fibular sesamoid, the transverse
inter-metatarsal ligament and the lateral capsule of
the first metatarso-phalangeal joint. The second
incision is made midline over the medial eminence
to remove the medial eminence and perform a
capsulorraphy. The proximal osteotomy is done
through a four-centimeter dorsal and longitudinal
third incision that starts over the base of the first
metatarsal and ends just proximal to the metatarso-
December 2006
KUWAIT MEDICAL JOURNAL
Table 2: Post-operative clinical results
Parameter
Result
n (%)
Subjective
Pain relief
Comfortable shoe fitting
Satisfaction with surgery
Objective
Excellent correction
Good correction
Recurrence
AOFAS hallux score
27 (90)
18 (60)
28 (93)
30 (80)
6 (15.7)
2 (5.3)
Average score 92 points,
range (81-97 points)
303
Table 3: Pre-operative versus post-operative clinical
assessment
Parameter
Pre-operative
assessment
n (%)
Post-operative
results
n (%)
Pain
30 (100)
03 (10) Mild pain p ≤ 0.05 significant
Shoe fitting problems
20 (67)
2 (7)
p ≤ 0.05 significant
Hallux valgus deformity 38 feet (100) 2 (5.3) Recurrence Highly significant
p < 0.01
Table 5: Post-operative complications
Complication
Table 4: Pre-operative versus post-operative radiological
findings
Parameter
Pre-op assessment
M (range)
HVA
1/2 IMA
DMAA
o
o
o
48 (43 -54 )
o
o
o
18 (16 -22 )
o
<100 in
13 feet (34%)
Tibial sesamoid
Medial in
0 feet
Shortening of 1st MTB --- NA
Dorsal angulation
--- NA
O-A1st MTP
--- NA
Post-op results
M (range)
o
o
o
13 (8 - 22 )
o
o
o
7 (5 -12 )
o
<100 in
34 feet (90%)
Medial in
28 feet (74%)
6.3% (1.7%-11%)
15 feet (39%)
One foot (2%)
Level of
significance
p ≤ 0.05 significant
p ≤ 0.05 significant
p ≤ 0.05 significant
p < 0.01 highly
significant
Not significant
p ≤ 0.05 significant
Not significant
M = mean NA= not available
cuneiform joint. The metatarsal osteotomy is begun
one to one and half centimeter distal to the
metatarso-cuneiform joint with the use of an
oscillating saw that has a curvilinear blade with the
concavity of the cut directed proximally (dome or
crescentic shaped osteotomy). The osteotomy is
displaced by retraction and pushing of the
proximal fragment medially and moving the distal
portion laterally with supination and rotation
around the proximal fragment. This usually results
in a lateral displacement of the distal portion by
about 3 - 5 mm to reduce the 1/2 IMA and correct
the metatarsus primus varus deformity of the 1st
metatarsal. The supination of the distal portion of
the metatarsal osteotomy and the great toe reduces
the sesamoids beneath the metatarsal head
correcting the great toe pronation, which mostly
accompanies severe hallux valgus. The site of
osteotomy is stabilized by either two K-wires (in
thirty feet) or by 4 mm cancellous screw (in eight
feet). The medial part of the joint capsule is repaired
with the great toe held in neutral dorsi-flexion
plantar-flexion position with slight varus over
correction. Through the second medial incision, the
extensor hallucis longus tendon is accessed and
lengthened by Z-plasty according to its tension
after the correction of hallux valgus deformity by
Level of
significance
Medial hypothesia of the hallux
Pin track infection
Deep infection
Mild under- correction
Recurrence of gross hallux valgus
Osteoarthritis 1st MTP
n (%)
Feet (%)
2 (6.6)
2 (6.6)
1
4 (13)
2 (6.6)
1
2 (5.3)
2 (5.3)
1
6 (15.7)
2 (5.3)
1
proximal osteotomy and the distal capsulorrphy
and lateral release. Post-operatively, the hallux is
protected in the corrected position by using P.O.P
slipper cast, which encases the hallux and foot
without immobilizing the ankle allowing its free
movements. The patient is allowed to walk from
the second post-operative day in the non-weight
bearing mode using crutches.
Follow-up:
The patients were followed-up for an average of
twenty-eight months (range 17- 47 months).
During the follow-up the cast and the K-wires were
removed 4-6 weeks post-operatively and the
patient started on a physiotherapy program for
active and passive dorsi-flexion and plantar flexion
exercises of the hallux and other toes. The patient
was allowed to bear weight partially and then fully
aided by crutches eight weeks post-operatively.
After 10-12 weeks post-operatively, the patients
discarded crutches and returned to normal
activities.
RESULTS
The results were categorized into subjective,
objective, radiological and complications.
A- Subjective results:
Out of all 30 patients (100%) who complained of
pain in their feet located primarily around the 1st
MP joint pre-operatively, only three had persistent
mild discomfort post-operatively (10%). Out of 20
patients (67%) with shoe-fitting problems preoperatively, 18 (90%) could be fitted with the same
shoe more comfortably post-operatively and 14
(70%) of these patients could even be fitted with a
304
Results of Combined Proximal Crescentic Metatarsal Osteotomy and Modified Distal Soft ..... December 2006
Fig. 2a
Fig. 2b
Fig. 2c
Fig. 2: Severe hallux valgus deformity with severe subluxation of the first metatarsophalangeal joint in the right foot of a 32 years old male patient
a. Pre-operative standing antero-posterior radiograph; b. Post-operative standing antero-posterior
radiograph; c. Final follow up radiograph after four years; d: Photograph of the right foot showing
satisfactory correction of the deformity.
narrower shoe.
The status of
two
patients
(10%) remained
unchanged
with regard to
the fitting of
shoes. Twentyeight patients
(93%)
were
satisfied with
the results of
surgery
and
the shape of
their foot or
feet. Two patients
(6.6%)
were
dissatisfied
with
the
operative
result due to
Fig. 2d:
recurrence of
the hallux valgus deformity to its pre-operative
magnitude and persistence of pain.
B- Objective results:
The hallux valgus deformity was corrected to a
clinically neutral hallux with regard to the valgusvarus deformity in 30 feet (80%). Six feet (15.7%)
had residual mild hallux valgus. Two feet (5.3%) in
two patients had recurrence of gross hallux valgus
post-operatively. Active dorsi-flexion of the first
MP joint averaged 50º with a range of 25º- 65º. The
average passive dorsi-flexion was 60 degrees with a
range of 30º-70º. The post-operative active plantar
flexion averaged 26 degrees with a range of 10-45
degrees and the passive average was 35 degrees
with a range of 15 - 50 degrees. There was residual
hallux pronation in three feet (18%) in three
patients (10%). The post-operative results are
shown in Table 2. The post-operative clinical
assessment has been further elaborated by using
the American Orthopedic Foot and Ankle Society
(AOFAS) hallux score[5,7,9]. The average score among
thirty patients in this study was 92 out of 100 points
with a range of 81- 97 points. A comparison of the
pre-operative assessment and post-operative
results is shown in Table 3.
C- Radiological Results:
The osteotomy site was united in all feet,
irrespective of the method of fixation. The HVA was
corrected an average of 35 degrees after the
procedure. The post-operative latest follow-up
average HVA was 13 degrees (range = 8 - 22
degrees) and it was less than 10º in 19 patients
(50%) with 26 feet (68.4%). 1/2 IMA was corrected
to an average of 11 degrees. The angle averaged 7º
(range 5º-12º) as shown in (Fig. 2: a, b, c) & (Fig. 3:
a, b, c). Post-operatively, the tibial sesamoid was
positioned medially in 28 feet (74%), centrally in
seven feet (18.5%) and laterally in the remaining
three feet (7.5%). In the latest postoperative weight
bearing antero-posterior foot radiograph, the
DMAA was corrected to <100º in 34 feet (90%) and
> 100º in four patients and the averaged DMAA
December 2006
Fig. 3a
KUWAIT MEDICAL JOURNAL
Fig. 3b
305
Fig. 3c
Fig. 3: Severe hallux valgus deformity with severe subluxation of 1st MTPjoint in the left foot of a
25 years-old female patient.
a. Preoperative standing antero-posterior radiograph; b. Postoperative standing antero-posterior
radiograph; c. Final follow up radiograph after three years; d. Photograph of the left foot-showing
correction of the deformity
was 9º The
subluxation of
1st MP joint
was corrected
in 35 feet (95%)
while it recurred
in two feet
(5%). The length
of 1st and 2nd
metatarsals
was measured
with
weight
b e a r i n g
radiographs to
Fig. 3d
determine
metatarsal
shortening after surgery. The method of measuring
first metatarsal shortening is shown in Fig. 4. The
percentage of shortening of the first metatarsal
averaged 6.3% (range = 1.7% - 11%) after the
osteotomy.
Post-osteotomy, the first metatarsal dorsal
angulation (elevation) malunion was noticed in 15
feet in 12 patients (40%). Dorsal angulation
occurred in four feet where the osteotomy was
fixed by 4.0 mm cancellous screw and in two of
them the angulation was noticed in the immediate
post-operative radiographs and in the other two,
the angulation was noticed during the late followup (50% of the osteotomies fixed by screws). Dorsal
angulation occured in 11 feet where the osteotomy
was fixed by K-wire (36.6% of the feet fixed by K-
wires), four of them noticed in immediate postoperative radiographs and the rest were observed
late in the follow-up. The osteoarthritic changes in
the 1st MTP joint noted, in latest follow-up in one
foot with narrowing of the joint space and
subchondral sclerosis. Acomparison of pre-operative
and post-operative radiological assessment is shown
in Table 4.
Complications:
Hypothesia on the medial aspect of the hallux
due to digital nerve injury was noted in two
patients (6.6%). In two patients (6.6%) where the
metatarsal osteotomy was fixed by K-wires, pin
track infection occurred which was cured by local
debridment and antibiotics. Deep infection
occurred in one patient (3.3%), which was treated
by wound debridment under general anesthesia
and antibiotics and this subsided with wound
healing three weeks after the debridment surgery.
No painful transfer metatarsalgia with or without
plantar keratosis under the head of second
metatarsal developed after surgery in any patient.
Recurrence of gross deformity occurred in two
feet (5.3%) in two patients (6.6%). Six feet (15.7%) in
four patients (13%) had mild residual deformity of
hallux valgus but the patients were satisfied with
the cure of pain and the cosmetic appearance of
their feet. Over correction with hallux varus
deformity was not noticed in any of the patients in
this series (Table 5).
306
Results of Combined Proximal Crescentic Metatarsal Osteotomy and Modified Distal Soft ..... December 2006
Fig. 4: Measuring first metatarsal shortening (X is the midpoint of AB.
The percentage of shortening of first metatarsal is then expressed as
X1/X2 pre-operative divided by X1/X2 at review x 100).
DISCUSSION
Selection of the operative technique for
correction of the bony deformities in hallux valgus
patients is mainly based on the first to second intermetatarsal angle (1/2 IMA). Severe deformity
where the 1/2 IMA is > 16º can be corrected using
proximal metatarsal osteotomies (proximal chevron,
crescentic, opening, and closing wedge osteotomy)
with distal soft tissue procedures [2,4,9]. Arthrodesis is
also advocated in severe painful hallux valgus[5].
Reported series show that success rates for the
proximal osteotomies are comparable, achieving
satisfactory results in the zone of 80 to 90%[7,9]. The
studies have shown, as well that those proximal
osteotomies may lead to substantial complications,
including first metatarsal elevation, metatarsal
shortening and transfer metatarsalgia due to
altered forefoot loading[3,11,12,13].
Regardless of adequate fixation of the first
metatarsal proximal osteotomy, dorsal angulation
has been reported to occur in the range of 28 - 82%
patients undergoing the procedures. Although this
angulation may occur as an intra-operative
technical failure, post-operative dorsi-flexion can
similarly occur as a result of early weight bearing
on a relatively unstable osteotomy. One of the big
advantages of proximal osteotomies is that it
achieves an actual instead of relative correction of
the intermetatarsal angle [3,5,7,11].
The crescentic basilar osteotomy, in particular,
has the problems of sagittal instability and postoperative first metatarsal dorsal angulation, most
likely due to poor osteotomy placement and
difficulty in fixation. But the technique still
provides a powerful tool to correct wide
intermetatarsal angles with minimal shortening.
One could also adjust the procedure in order to
obtain exact correction without additional wedging
and facilitate triplanar correction by angling the
osteotomy in various directions. The rate of first
metatarsal dorsal angulation was 39% in this study
distributed among the cases fixed by K-wires
(36.6%) and osteotomies fixed by screws (50%) with
a difference which does not reflect any statistical
significance. However, none of the patients
developed transfer metatarsalgia, most likely due
to low incidence of first metatarsal minimal
shortening (average of 6.3%). One of these complications
aggravates the other in that if there is both
shortening and dorsi-flexion, the problem of a
transfer lesion is compounded. There are times
when dorsi-flexion occurs with minimal shortening
and no problem results[15,17].
In 1982, Cedell and Astrom reported the results
of a basal dome osteotomy and distal soft tissue
procedure in forty-six feet. The results were
excellent in 78% of the feet and good in 11%[12,13]. In
1992, Mann reported the results of proximal
Crescentic osteotomy with distal soft-tissue repair
in seventy-five patients (109 feet). A majority (93%)
of the patients were satisfied with the surgery[18,19].
In our series, 93% patients were satisfied with the
outcome of surgery. Excellent correction of the
severe hallux valgus was achieved in 79% patients
and good correction in 16% patients with average
AOFAS hallux score of 92 points (range = 81-97
points). This conforms to the results of Dome
osteotomy and distal soft tissue procedures in the
literature. However, most of the literature reports
had a heterogeneous group of mild, moderate and
severe hallux valgus. To the best of our knowledge,
this is the first series of only severe hallux valgus
treated by proximal dome osteotomy, distal soft
tissue lateral release and medial repair[3,4,13,20]. The
modification of adding Z-plasty of the extensor
hallux longus tendon to the distal soft tissue
procedure (to reduce the possibility of recurrence
by decreasing the bowstring effect of the EHL after
deformity correction by osteotomy) may play a role
in having only two cases of recurrence in this series
of severe hallux valgus after surgery.
December 2006
KUWAIT MEDICAL JOURNAL
The rate of permanent complications in this
series was in four patients (13%) but none of our
patients complained of transfer metatarsalgia with
or without plantar callosity beneath the second
metatarsal head and only one patient had
osteoarthritis in the 1st MTP joint. The rate of
complications in this study is very similar to what
is mentioned in other reports in the literature[7,9,21,22].
Proximal crescentic metatarsal osteotomy with
distal soft tissue procedure modified by extensor
hallucis longus Z-plasty has proved effective in
relieving symptoms and in restoring feet
appearance in severe hallux valgus deformity to
nearly normal shape and function with a low rate of
recurrence and other complications.
The
significance of the impact of our distal soft tissue
modification in hallux valgus correction surgery
will need further evidence by planning a
randomized prospective study.
CONCLUSION
We believe according to the results of this study
and other reports in the literature that the proximal
crescentic metatarsal osteotomy combined with
distal lateral release, medial repair and lengthening
of the EHL is a reliable and successful surgical
technique in treating severe hallux valgus deformity
in adult feet. The technique is simple, has a low rate
of complications and is associated with durable
correction relieving the patients’ symptoms enough
to justify its recommendation.
ACKNOWLEDGEMENT
We would like to express our thanks to Dr Samir
AbdAlRazek, Head, Department of Orthopedics,
Al Razi Hospital for his great support. We also
appreciate the help rendered to us by Dr Gehan
Baker, Dr Mohamed Baker, Dr Montasser Bashir, Dr
Osama Sobhy and Dr Hazem Hantera for their
great support.
5.
6.
7.
8.
9.
10.
11.
12.
13.
14.
15.
16.
17.
18.
19.
REFERENCES
1.
2.
3.
4.
Carr CR, Boyd BM. Correctional Osteotomy for metatarsus
primus valgus. J Bone Joint Surg 1968; 50-A:1353-1367.
Bargman J, Corless J, Gross AE, Lange F. A review of
surgical procedures for hallux valgus. Foot Ankle 1980;
1:39-43.
Donick II, Berlin SJ, Block LD, Costa AJ, Fox JS, Martorana
VJ. An approach for hallux valgus surgery-fifteen years
review, part II. J Foot Surg 1980; 19:171-184.
McBride ED. The McBride bunion hallux valgus operation.
Refinements in the successive surgical steps of the
operation. J Bone Joint Surg 1967; 49-A:1675-1683.
20.
21.
22.
307
Kernozek TW, Elfessi A, Sterriker SA. Clinical and
biomechanical risk factors of patients diagnosed with
hallux valgus. J Am Podiat Med Assoc 2003; 93:97-103.
Breslauer C, Cohen M. Effect of proximal articular set
angle-correction osteotomies on the hallucal sesamoid
apparatus: a cadaveric and radiographic investigation. J
Foot Ankle Surg 2001; 40:366-373.
Mc Cluskey LC, Johnson JE, Wynarsky GT, Harris GF.
Comparison of stability of proximal Crescentic metatarsal
osteotomy and proximal horizontal “V” osteotomy. Foot
Ankle Int 1994; 15:263-270.
Smith RW, Reynolds JC, Stewart MJ. Hallux valgus
assessment. Report of research committee of American
Orthopedic Foot and Ankle Society. Foot Ankle 1984; 5:92103.
Trnka HJ, Muhlbawer M, Zembsch A, Hungerford M,
Ritschl P. Basal closing wedge osteotomy for correction of
metatarsus varus: 10 to 22 years follow-up. Foot Ankle Int
1999; 20:171-177.
Groulier P, Currale G, Prudent HP, Vedel F. Result of
treatment of hallux valgus with modified McBride
operation with or without supplementary phalangeal or
metatarsal osteotomy. French J Orthop Surg 1988; 2:412421.
Easley ME, Kiebzak GM, Davis WH, Anderson RB.
Prospective randomized comparison of proximal crescentic
and proximal chevron osteotomies for correction of hallux
valgus deformity. Foot Ankle Int 1996; 17:307-316.
Shaw AH, Pack LG. Osteotomies of the first ray for hallux
abudcto- valgus deformity. J Am Podiatr Med Assoc 1974;
64: 567-580.
Mann RA, Coughlin MJ. Hallux valgus - etiology, anatomy,
treatment and surgical considerations. Clin Orthop 1981;
157:31-41.
Michael J, Coughlin B, Idaho. Hallux valgus: An
instructional course lecture, The Am Academy of
orthopedic surgeons. J Bone Joint Surg 1996; 78:932-966.
Cohen M, Roman A, Ayres M, Freedline A. The crescentic
shelf osteotomy. J Foot Ankle Surg 1993; 32:209-226.
Carpenter B, Motley A. Adding stability to the crescentic
basilar metatarsal osteotomy. J Am Podiatr Med Assoc
2004; 94:5.
Cedell CA, Astrom M. Proximal metatarsal osteotomy in
hallux valgus. Acta Orthop. Scandinavia 1982; 53:1013-1018.
Resch Sylvia, Stenstrom Anders, Eguard Nils. Proximal
closing wedge osteotomy and abductor tenotomy for
treatment of hallux valgus. Foot Ankle 1989; 9:272-280.
Johnson JE, Clinton TO, Boxter DE, Gottlieb MS.
Comparison of chevron osteotomy and modified McBride
bunionectomy for correction of mild to moderate hallux
valgus deformity. Foot Ankle 1991; 12:61-68.
Jones KJ, Feiwell LA, Freedman EL, Cachiolo A. The effect
of chevron osteotomy with lateral capsular release on the
blood supply to the first metatarsal head. J Bone Joint Surg
1995; 77- A:197- 204.
Mann RA, Sally Rudicel, Graves SC. Repair of hallux valgus
with a distal soft tissue procedure and proximal metatarsal
osteotomy. J Bone Joint Surg 1992; 74-A:124-129.
Mann RA. Distal soft tissue procedures and proximal
metatarsal osteotomy for correction of hallux valgus
deformity. Orthopedics 1990; 13:1013-1018.
KUWAIT MEDICAL JOURNAL
December 2006
Original Article
Safety of Laparoscopy in Acute Cholecystitis
Wael Fathi Hassaniah, Mohamed Al Haifi, Talib Jumaa
Department of Surgery, Al Amiri Hospital, Kuwait
Kuwait Medical Journal 2006, 38 (4): 308-310
ABSTRACT
Objective: Laparoscopic Cholecystectomy (LC) is the
gold-standard procedure for chronic cholecystitis.
However, its safety in acute cholecystitis has been
questioned because of the abnormal anatomy associated
with the acute inflammation. Our aim was to evaluate
the safety of LC in acute cholecystitis.
Design: Retrospective
Setting: Department of Surgery, Al-Amiri Hospital,
Kuwait
Material and Methods: During the period 1992 -1999,
300 patients with acute cholecystitis were evaluated. We
assessed the efficacy of LC by studying the postoperative
hospital stay; and its safety by studying the rate of
conversion, especially by adopting the policy of early
conversion whenever the anatomy was obscure. The
morbidity associated with LC in acute cholecystitis was
evaluated.
Results: Postoperative hospital stay was one day in 45%
and two days in 23% patients. Our conversion rate was
15%. Major postoperative complications were seen in 4%
cases. There was no incidence of CBD injury.
Conclusion: LC is a safe and effective procedure for acute
cholecystitis if the policy of early conversion when
anatomy is obscured is adopted.
KEYWORDS: acute cholecytitis, common bile duct injury, laparoscopic cholecystectomy
INTRODUCTION
Laparoscopic Cholecystectomy (LC) is now
considered as the procedure of choice for patients
with gall bladder disease, especially those with
chronic cholecystitis[1,2] due to reduced postoperative
hospital stay and early return to work. However, in
acute cholecystitis (AC), the presence of edema and
inflammation that results in obscuring the anatomy,
make the operative dissection much more difficult
and this could result in higher morbidity and
reduced benefit from the laparoscopic approach[3,4].
In our experience, LC for AC is a safe and effective
method for management of AC with an acceptable
rate of conversion and morbidity[5,6]. This has been
accomplished by a low threshold for conversion
when anatomy is distorted.
MATERIALS AND METHODS
Two thousand seven hundred and fifty patients,
who underwent LC from February 1992 until October
1999, were retrospectively evaluated. Three hundred
patients presented with acute cholecystitis. The
diagnosis was based on history, clinical examination,
the presence of fever, leucocytosis and diagnostic
evidence of AC by ultrasound examination. Operative
time, conversion rate, the reasons for conversion and
postoperative complications were evaluated in
both urgent and emergency cases.
Technique:
LC was done by using the four port technique.
A needle aspiration of the gall bladder was done at
the beginning of the procedure to facilitate
grasping the gall bladder wall which is usually
thickened due to the inflammation. Omental
adhesions were released by blunt dissection to
identify the Callot’s triangle. If traction of the
Hartman’s pouch was not feasible by the usual
graspers, we used the Wolf grasper which has a
good grip on the wall by the sharp stems. Traction
on the fundus was facilitated by a stitch which was
then caught by a grasper. If the dissection at the
Callot’s triangle was difficult, then an attempt was
made at identifying the structures first by fundus
dissection. Electrocautery dissection was used to
expose the cystic duct and the cystic artery. This
was facilitated by the use of hydro-dissection with
the suction tube. For thick and wide cystic ducts, a
Roeder loop knot was used to secure them. We did
not do routine intra-operative cholangiogram.
Patients with raised liver enzymes or suspected of
having common bile duct stones had a preoperative endoscopic retrograde cholangiopancreatogram (ERCP)[7,8,9]. The gall bladder and
any spilled stones were collected in a retrieval bag
which was extracted through an extended
umbilical port. Draining the liver bed was not done
Address correspondence to:
Dr Wael Fathi Hassaniah, PO Box 1002 - Hawalli, Kuwait. E-mail: [email protected]
December 2006
KUWAIT MEDICAL JOURNAL
Table 1: Reasons for prolonged hospital stay (more than
one day)
Reason
Conversion
Gall bladder pathology
Patient’s request
Complications
No. of cases
45
50
15
27
309
Table 2: Reasons for conversion
Reason for conversion
Gall bladder pathology
Abnormal anatomy
Bile leak and stone spillage
Abdominal adhesions
Cystic artery bleeding
Common bile duct injury
Bowel injury
No. of cases
35
20
15
4
2
0
0
Table 3: Operative complications
Complication
Bleeding
Common bile duct injury
Cystic duct injury
G B puncture
Liver trauma
No. of cases
12
Nil
4
45
6
routinely and it’s use was left to the judgement of
the operating surgeon.
RESULTS
LC was attempted in 300 patients with a clinical
and radiological diagnosis of AC. Out of these
patients, 120 (40%) were male and 180 (60%) female.
The mean age was 45 years (range 17 - 73 years).
The mean operating time was 80 minutes (range 45
- 310 minutes). The mean postoperative hospital
stay was 1.56 days (range 1 - 20 days). One day
postoperative hospital stay was seen in 137 (45%)
and two days hospital stay in 69 (23%) patients. The
remaining patients stayed for more than two days.
The reasons of prolonged hospital stay (more than
one day) are shown in Table 1. In some cases, there
was more than one reason to account for the
increased hospital stay. The conversion rate was
15% (45). The reasons for conversion are shown in
Table 2. There was again more than one reason for
conversion to open cholecystectomy.
Pre-operative ERCP was done in 42 cases. The
indications were raised liver function tests or
evidence of dilated common bile duct by ultrasound.
ERCP was abnormal in only 20 (47%) cases where
stones were found and extracted. Postoperative
ERCPwas done in eight cases and was abnormal in
seven (87%) cases. Postoperative ERCPwas done to
deal with retained stones (2 cases), postoperative
complications such as bile leak (3 cases) and
pancreatitis (2 cases). Our operative complications
are shown in Table 3, and postoperative
complications in Table 4.
Re-admission to hospital was considered as a
minor complication and was seen in 11 cases; out
of which two cases were due to retained stones,
three cases were found to have small non-drainable
Table 4: Post-operative complications
Complication
Major complications
Common bile duct Injury
Bleeding
Bile leak
Abdominal collection
Melena
Pancreatitis
Minor complications
Re-admission
Wound Complications
Others:
Medical or anesthesia related
No. of Cases
Nil
1
3
5
1
2
11
20
15
abdominal collection, two cases due to non-specific
abdominal pain and four cases due to upper
abdominal pain that was due to peptic ulcer. Other
minor complications included those due to
anesthesia or associated medical disease like
ischemic heart disease, heart failure and
hypertension.
DISCUSSION
Laparoscopic cholecystectomy done electively
has significant benefits for the patients, including
short hospitalization and reduced wound complications.
In our experience, these benefits have also been
achieved for patients with acute cholecystitis,
where the majority of our patients stayed postoperatively for short periods (45% stayed for one
day and 23% stayed for two days). Twenty (6.6%)
patients suffered from minor wound complications
like wound seromas or superficial wound infection.
The presence of edema, inflammation, fibrosis
and sometimes necrosis with gangrene make
dissection of the Callot’s triangle and the gall
bladder more difficult, especially if associated with
omental adhesions. This can lead to more
procedure-related complications. An aspiration
needle can be used to decompress the edematous
and thick-walled gall bladder which would
facilitate grasping the wall. Also, the use of stronger
tooth graspers for the cephalad fundus retraction
helped. For thickened cystic ducts, the use of extra
310
Safety of Laparoscopy in Acute Cholecystitis
large clips or roeder loop and the use of a bag for
retrieval of the gall bladder through an extended
umbilical port is useful. Closed suction drainage of
the liver bed was performed in cases with bile
leakage, spilled stones, presence of extensive
necrosis in the liver bed and in cases with thickened
cystic duct where there is a potential for bile leak. In
spite of this modified technique the anatomy
remains unclear; therefore a low threshold for
conversion should be maintained to avoid serious
complications, especially common bile duct injury[10].
Our conversion rate was 15% and is similar to the
conversion rates in published literature[11,12].
Our postoperative complications rate was 19.3%.
However, major complications were only 4% as
shown in Table 4. We had no common bile injury
and only one case of intra- abdominal bleeding that
was from the liver bed. This patient required a
laparotomy. We had three cases of bile leak, two
cases from cystic duct and one case from gall
bladder bed. All cases were managed conservatively
by ERCP and percutaneous aspiration of the
collection under ultrasound guidance [13,14]. One
patient had malena after ERCP. Abdominal collection
was seen in five cases. Three were managed
conservatively and in two patients, aspiration
under ultrasound guidance was done[15].
CONCLUSION
Laparoscopic cholecystectomy for acute cholecystitis
is an effective procedure due to reduced
postoperative hospital stays and wound complications.
It is also safe due to reduced postoperative
morbidity and with an acceptable rate of
conversion. This is achieved by a policy of early
conversion in cases where the anatomy is not clear.
REFERENCES
1.
Schirmer BD, Edge SB, Dix J, Hyser MJ, Hanks JB, Jones RS.
Laparoscopic cholecystectomy: Treatment of choice for
symptomatic cholelithiasis. Ann Surg 1991; 213:665-676.
2.
3.
4.
5.
6.
7.
8.
9.
10.
11.
12.
13.
14.
15.
December 2006
Anderson RE, Hunter JG. Laparoscopic cholecystectomy is
less expensive than open cholecystectomy. Surg Laparosc
Endosc 1991; 1:82-84.
Cuschieri A, Dubois F, Mouiret P, Becker H, Buess G, et al.
The European Experience with laparoscopic cholecystectomy.
Am J Surg 1991; 161:385-387.
Kum CK, Goh PM, Isaac JR, Tekant Y, Ngoi SS.
Laparoscopic cholecystectomy for acute cholecystitis. Br J
Surg 1994; 81:1651-1654.
Lujan JA, Parrilla P, Robles R, Marin P, Torralba JA, GarciaAyllon J. Laparoscopic cholecystectomy vs open cholecystectomy
in the treatment of acute cholecystitis: a prospective study.
Arch Surg 1998; 133:173-175.
Eldar S, Sabo E, Nash E, Abrahamson J, Matter I.
Laparoscopic cholecystectomy for acute cholecystitis:
prospective trial. World J Surg 1997; 21:540-545.
Phillips EH: Controversies in the management of common
duct calculi. Surg Clin North Am 1994; 74:931-948.
Fernandez M, Csendes A, Yarmuch J, Diaz H, Silva J.
Management of common bile duct stones: the state of the
art in 2000. Int Surg 2003; 88:159-163.
Liu CL, Fan ST, Lai EC, Lo CM, Chu KM. Factors affecting
conversion of laparoscopic cholecystectomy to open
surgery. Arch Surg 1996; 131:98-101.
Lo CM, Fan ST, Liu CL, Lai EC, Wong G; Early decision for
conversion of laparoscopic to open cholecystectomy for
treatment of acute cholecystitis. Am J Surg 1997; 173:513517.
Johansson M, Thune A, Blomqvist A, Nelvin L, Lundell L.
Management of acute cholecystitis in the laparoscopic era:
results of a prospective, randomized clinical trial. J
Gastrointest Surg 2003; 7:642-645.
Cox MR, Wilson TG, Luck AJ, Jeans PL, Padbury RTA,
Toouli J. Laparoscopic cholecystemy for acute inflammation
of the gall bladder.Ann Surg 1993; 218:630-634.
Mehta SN, Pavone E, Barkun JS, Cortas GA, Barkun AN. A
review of the management of post cholecystectomy bile
leak during the laparoscopic era. Am J Gastroenterol 1997;
92:1262-1267.
Bose SM, Mazumdar A, Singh V. The role of endoscopic
procedures in the management of post-cholecystectomy
and post-traumatic biliary leak. Surg Today 2001; 31:45-50.
Lee VS, Chari RS, Cucchiarro G, Meyers WC.
Complications of laparoscopic cholecystectomy. Am J Surg
1993; 165:527-532.
December 2006
KUWAIT MEDICAL JOURNAL
Insight
Computerization in Primary Care: an Insight
Huda I Al-Shaibani1, Siham YF Al-AbdulGhafour2, Amal H Al-Saqabi3
Al-Shiab Primary Health Care Centre, Hawalli, Kuwait
2
Primary Health Care, Hawalli, Health Area, Kuwait
3
Sabah Al Salim North Primary Care Centre, Kuwait
1
Kuwait Medical Journal 2006, 38 (4): 311-314
ABSTRACT
We present our experience with the first year of
computerization in the Primary Health Care (PHC)
Centers in Hawalli Health Area. Diagnoses were entered
according to the ICD-10 Classification by PHC
Physicians. Data could be retrieved from eight centers.
The percentage of recording was calculated and diseases
were tabulated under different body systems. Out of 1.5
million visits received, only 0.7 million were entered
(47%), with considerable variations among different
centers (15-84%). The great majority of visits entered
(88%) were for acute conditions. Eighty-six thousand
visits (12%) were for chronic conditions, of which
diabetes (28%) and hypertension (13%) were the
commonest. Difficulties leading to the low percentage of
recordings were: insufficient users’ training, system
closure during holidays, slow response to users or
maintenance needs and shortage of supportive
personnel. Despite these difficulties, we consider the
experience as promising. The PHC Physicians have the
impetus to improve. We could develop an idea on the
pattern of illnesses dealt with in PHC centres. The
potential for improving patient care, research and
planning, based on the critical appraisal of retrieved data
is discussed. The need to have emphasis laid on
organizational issues and users’ needs, rather than
merely on administrative and financial issues, is
highlighted.
KEY WORDS: automated database, database information retrieval, research in general practice.
INTRODUCTION
During the 1980s and 1990s, general practices
including primary care, have increasingly become
computerized[1], might reach over eighty percent
before the turn of the century[2].A great potential for
this development in boosting epidemiologic
research and patient care was lately realized [2].
Databases provide an efficient means of storing
and retrieving large amounts of well-structured
data[3]. Health professionals need to become skilled
in the critical appraisal and interpretation of
reports based on the collection of these data and
their use in policy making [4]. Computers were
introduced in the primary health care (PHC)
centers in Hawalli Health Area in 2003. Physicians
started entering patients’ information in 2004,
following one session of demonstration. Implementing
electronic medical records (EMR) requires a
substantial start up effort and ongoing training at
the practice site [5], with emphasis laid on
organizational issues and users’ problems rather
than merely on devices[6]. We herein report our
experience with the first year of computerization in
our PHC centers. The basic epidemiologic features
of diseases dealt with in those centers are
highlighted. Limitations and areas where there is a
place for improvement are discussed and the
potential for research in PHC setup, based on the
retrieval and use of computer based data is
emphasized.
METHODS
We analyzed the computer-based records from
eight of the 13 PHC centers in Hawalli Health Area.
Five centers were not included in the study for the
following reasons: incomplete information in one,
no computerization in two and renovation of other
two centers. A permission to conduct such analysis
was officially obtained from the Area Director. The
unanimity and confidentiality of patients were
protected as the analysis was restricted to the
diagnoses made without reference to patients’
specifications. A computer print was forwarded to
the Head of Primary Care (a co-author) from each
of the eight PHC centers. It contains the number of
patients with specific diagnoses entered according
to the ICD-10 diagnostic code and tabulated under
various body systems and other headings.
Address correspondence to:
Dr. Huda I Al-Shaibani, P.O. Box 24169 Safat 13103 Kuwait. Tel: 5524364
312
Computerization in Primary Care: an Insight
December 2006
Table 1: Percentage of computer entry in eight primary
health care centres in Hawalli Health Area during 2004
Table 2: The leading ten diagnoses in primary health care
centers in Hawalli Health Area during 2004
PHC Centre
Order
Total no. of
No. of visits
Percentage
visits
entered in EMR* of computerization
Salwa
317,500
Salmiyah West
291,426
Sabah Al-Salim South 209,606
Jabriyah
196,210
Rumithiyah
196,183
Bayan
154,689
Meshrif
115,543
Al-Shiab
37,933
Total
1519,090
139,729
146,535
118,754
37,957
29,801
113,710
93,813
31,944
712,243
44
50
57
19
15
74
81
84
47
* EMR: Electronic medical records
The percentage of computer entry in individual
PHC centers was calculated as the ratio of the
number of visits entered to the actual number of
visits received by the centers. The actual numbers
of visits were obtained from the annual report of
Hawalli Health Area[7]. The quality of recording has
not been examined. The obstacles leading to
incomplete entry of patients’ data have been
periodically reported to one of the authors.
The total number of cases entered under various
body systems was calculated, and only the leading
five systems were presented for the sake of
simplicity. For the same reason we presented the
leading ten diagnoses, out of about 500 listed. An
attempt was made to identify chronic conditions
generally known to be associated with morbidity
and/or mortality, from acute and trivial conditions,
as well as conditions listed under communicable
disease. Only univariate analysis was performed
using numbers and percentages to show the
frequency of various entities, as we do not have a
comparative set of data on which we can apply
multivariate analysis.
RESULTS
The total number of visits seen in the area was
approximately 2.3 million, of which 1.52 million
were seen in the eight PHC centes where the study
took place[7]. Of these, 712,243 visits were actually
entered in the computer by 103 PHC physicians
(47%). This low rate of entry can be attributed to
several factors: frequent breakdowns and delay of
maintenance, the lack of follow-up demonstrations,
the shutting down of the system during weekends
and public holidays, and the very short consultation
time during rush hours.
Individual PHC centers varied considerably in
the percentage of computer entry (Table 1), between
15 and 84 percent. Centers with the lowest rate of
1
2
3
4
5
6
7
8
9
10
Diagnosis
Number
entered
Percent
from total
Upper respiratory infections
Bronchial asthma
Bronchitis
Hypertension
Gastroenteritis
Allergic rhinitis
Muscle spasms and cramps
Conjunctivitis
Diabetes
Backache
Subtotal
241,269
34,499
26,618
23,894
21,934
18,488
14,477
12,884
11,662
11,091
416,816
33.9
4.8
3.5
3.4
3.1
2.6
2.0
1.8
1.6
1.6
58.3
entry are those open on weekends and public holidays,
each serving 3-4 residential areas. Computers could
not be used as the PHC centers were not
interconnected during 2004. This problem was
solved in 2005.
The leading ten diagnoses are depicted in Table
2, and they constituted 58 percent of the entered
workload. Four of these, first to third and sixth
were respiratory illnesses. Eight of these illnesses
are trivial and only two (diabetes and hypertension)
are associated with mortality or morbidity.
The total number of cases entered in the
computer under the leading five body systems is
shown in Table 3. Respiratory system disorders
were responsible for 46 percent of the total
workload, followed by the digestive system (8%).
Non-morbid conditions (examinations for school
entry, for joining sports, vaccination, etc) accounted
for 15 percent of cases, leaving 15 percent for all
other systems.
Thirty diagnoses, chosen because they are
associated with mortality and/or morbidity and
need chronic care, were responsible for a total of 86,
494 entered visits (12%). The leading diagnoses are
depicted in Table 4. The remaining 88% of cases
entered were acute, mostly trivial conditions, and
consumed over 80 percent of time available for
primary care practitioners to practice acute,
preventive and chronic care.
Only 3,715 incidents of communicable diseases
were recorded (Table 5), and 90 percent of these
were due to chickenpox. There were only three
cases of whooping cough and 17 cases of tuberculosis.
Of particular interest is the finding of 194 records of
gonococcal infections.
The incomplete patient information and the low
percentage of computer entry (47%), both precluded
the estimation of prevalence and incidence rates as
well as the reporting on mortality or morbidity
statistics.
December 2006
KUWAIT MEDICAL JOURNAL
Table 3: The leading five body systems under which
diagnoses were entered in the computer records of eight
primary health care centres in Hawalli Health Area in
2004
No. of Cases
Percent
Respiratory system
Digestive system
Skin
Musculo-skeletal system
Cardiovascular system
325,593
56,199
44,741
44,522
28,180
46
8
6
6
4
Subtotal
499,235
70
Table 5: Visits due to communicable diseases in eight
primary health care centres during 2004
Disease
Chickenpox
Gonococcal infections
Mumps
Rubella
Measles
Tuberculosis
Whooping cough
Total
Number
3,352
194
75
50
24
17
3
3,715
DISCUSSION
The low recording rate of 47 percent (Table 1)
was not unexpected in view of difficulties
encountered during the initial implementation.
Users’ training was limited to a single session of
demonstration, the system used to be shut down
during holidays, and the responses to maintenance
and user requests were not prompt. In three centers
however, the rate of recording exceeded 70 percent
(Table 1), an evidence that PHC physicians have the
impetus to improve on this issue. These difficulties
have long been recognized[5], as initial implementation had laid emphasis on devices rather than
organizational issues[6]. Financial and administrative
restraints compromised optimal utilization of the
system[6], which must be primarily targeted at the
user, as the time needed to adequately train him is
substantial[8]. He should be supported by the
introduction of clinical decision support systems,
which provide him with useful information
regarding diagnosis, therapy and prognosis [8, 9].
Computers have great potential for epidemiologic
research[2] and promote more effective patient care
by reliably and effectively storing and retrieving
patient data[3,4,8,9]. We were able to develop an idea
on the pattern of health problems in our PHC
centers (Tables 2-5), and the opportunities for
research in PHC centers should be enhanced. The
physician is an information manager, who processes,
313
Table 4: Morbid conditions that need chronic care and
carry mortality and morbidity risks
Morbid condition(s)
Hypertension
Diabetes
Chronic arthritis
Hypercholesterolemia and obesity
Migraine
Heart disease
Other 24 diagnoses
Total
Number
23,839
11,662
4,893
2,570
2,421
1,041
40,068
86,494
retrieves and applies information related to all
aspects of patient management[10]. Hence, his
information needs must be met[8,11]. This may entail
finding the relevant resources, mastering new and
multiple applications and ensuring ongoing
education[8].
Family practice has been slowly but steadily
dominating primary care in Kuwait [13]. Acute
problems were responsible for 88 percent of visits
to our PHC centers (Tables 2, 3), compared to 58
percent reported elsewhere[14]. It is well known that
acute care cannot be deferred[12], hence, time
available for chronic care is compromised[8,12]. It is
less than 10 minutes in our PHC centers[7] and
compares poorly with an average of 20 minutes
recommended to complete a chronic care visit[12], of
which 86 thousand cases were entered. This may
reflect negatively on the quality of care as well as on
the efficiency of data recording.
We have so far, not encountered issues related to
the inherent threat to patients’ privacy and
confidentiality, usually due to unauthorized access
to patient information [15]. This is particularly
relevant to sexually-transmitted diseases like
gonococcal infections (Table 5), and epilepsy, to
mention examples. This important issue needs to be
considered, as lack of confidentiality could lead to a
breakdown of doctor-patient relationship[1,15].
We believe the introduction of computerization
is a leap forward and the first year of
implementation was a success despite limitations.
Physicians in PHC centers are encouraged to
retrieve, collect and use stored data for improvement
of care as well as for research. Policy makers need
to develop a critical appraisal of retrieved data and
reports based on this retrieval and use this in
planning. We recommend that health authorities
lay more emphasis on users’ needs. This includes
ongoing training at the practice site, provision of
expert advice and meeting his information needs,
particularly, clinical decision support systems.
314
Computerization in Primary Care: an Insight
ACKNOWLEDGMENT
The authors wish to thank Dr Muhammed AlAyyad, Director, Hawalli Health Area for his
encouragement and support and the 103 primary
health care physicians who painstakingly managed
to enter patient data. Our thanks to Dr Faisal AF ElKhuffash, consultant paediatrician, Mubarak AlKabeer Hospital for his continued help and support
during the preparation of the manuscript.
10.
REFERENCES
11.
1.
2.
3.
4.
5.
Ridsdale L, Hudd S. Computers in the consultation: the
patient’s view. Br J Gen Practice 1994; 44:367-369.
Walton R, Randall T. Communication in the year 2000. Br J
Gen Practice 1994; 44:434-435.
Wyatt J. Computer-based Knowledge Systems. Lancet 1991;
338:1431-1436.
Heller RF, Page I. A population perspective to evidencebased medicine: evidence for population health. J
Epidemiol Community Health 2002; 56:45-47.
Ariza AJ, Binns HJ, Christoffer KK. Evaluating computer
capabilities in a primary health care practice-based research
6.
7.
8.
9.
12.
13.
14.
15.
December 2006
networks. Ann Fam Med 2004; 2:418-420.
Wyatt JC. Hospital information management: The need for
critical leadership. Br Med J 1995; 311:175-180.
Al-Abdulghafour SYF. Annual Report, 2004. Hawalli
Health Area.
Westberg EE, Miller RA. The basis for using the internet to
support the information needs of primary care. J Am Med
Inform Assoc 1999; 6:6-25.
Weisman F, Hasman A, van den Herik HJ. Information
retrieval: State of the art. Int J Med Inform 1997; 47:5-26.
Levinson DJ. Information, computers and clinical practice
(commentary). Am J Med Assoc 1983; 5: 607-609.
Covell DG, Uman GC, Manning PR. Information needs in
office practice: are they being met? Ann Int Med 1985;
103:596-599.
Ostbye T, Yarnall KSH, Krayse KM, Pollak Kl, Gradison M,
Michener JL. Is there time for management of patients with
chronic disease in primary care? Ann Fam Med 2005; 3: 209214.
Fraser RG. Developing family practice in Kuwait. Br J Gen
Practice 1995; 45: 102-105.
Stange KC, Zyzanski SJ, Jean CR, et al. Illuminating the
‘black box’. A description of 4454 visits to 138 family
physicians. J Fam Practice 1998; 46:377-389.
Carman D, Britten N. Confidentiality of medical records:
the patients perspective. Br J Med Practice 1995; 45:485-488.
December 2006
KUWAIT MEDICAL JOURNAL
Case Report
Neuronal Ceroid Lipofuscinoses: Report of Five Cases in
Kuwait
Maliha Askar Soud Al-Bloushi 1, Jehoram T Anim 2, Yousif Kasim Habeeb 1
Department of Pediatrics, Neurology Unit, Mubarak Al-Kabeer Hospital, Kuwait
2
Department of Pathology, Faculty of Medicine, Kuwait University, Kuwait
1
Kuwait Medical Journal 2006, 38 (4): 315-320
ABSTRACT
We report upon five children with neuronal ceroid
lipofuscinoses diagnosed over an eight year period (19962004) in the pediatric neurology unit of a tertiary service
hospital in Kuwait. Three cases were diagnosed by
lysosomal enzymes while the two other cases were
confirmed by skin biopsy. Although molecular genetic
studies, when available, allow for definitive diagnosis,
ultrastructural studies of skin biopsy material are simple
available alternative. We feel that this disorder is under
diagnosed and skin biopsies should be utilized when this
disorder is considered.
KEYWORDS: neuronal ceroid lipofuscinoses, neurodegenerative disease, skin biopsy
INTRODUCTION
Neuronal ceroid lipofuscinoses (NCLs) constitute
the most common group of progressive
neurodegenerative diseases in children with an
autosomal recessive inheritance[1,2]. Clinicopathologic
and genetic studies have proved that NCLs
constitute a group of highly heterogeneous disorders[3,4].
The precise cause remains undetermined but all
available evidence suggest an inborn error of
metabolism[5]. The NCLs include eight forms that
result from genetic deficiency on genes CLN (1) to
CLN (8) [6]. Four classic forms which include
infantile (INCL), late infantile (LINCL), juvenile
(JNCL) in addition to adult (ANCL) form and four
variants of LINCL[6]. The disease is characterized by
visual impairment, progressive myoclonic epilepsy,
decline in cognitive and motor skills resulting in
premature death[1,7,8]. The course reflects progressive
neurodegeneration. The diagnosis is usually made
based on demonstration of autoflourescent lysosomal
lipopigment in rectal biopsies and skin biopsies[9,10].
With recent advances in molecular genetics,
diagnosis of certain subtypes is possible, without
the need for invasive procedures like rectal
biopsies. Thus, prenatal diagnosis became an
option.
CASE REPORTS
Case 1
BA was the first born male child of a young
Kuwaiti couple who are distant relatives. He had
uneventful pre and perinatal periods. He was born
at term weighing 3 kg. He was seen at nine months
and was considered entirely normal although his
parents thought he had poor eye contact and
appeared socially indifferent. There was some
concern regarding his development; although he
sat independently at eight months and walked
unassisted at 16 months, he did not respond
appropriately to verbal stimuli. He was first seen
by a neurologist at the age of 22 months. By this
time he was showing signs of regression as he had
lost some of his acquired milestones: stopped
walking independently, lost speech (he used to say
up to three words), stopped laughing when tickled
and lost some manual skills such as waving good
bye.
Examination revealed no dysmorphic features.
He was socially indifferent with no eye contact and
an expressionless child. His weight was on the 20th
centile, length on the 40th centile but he had
microcephaly (below the 3rd centile). Few myoclonic
jerks were noted during examination. Ophthalmologic
examination was normal including both fundi.
Cranial nerve examination was normal. He could
sit unsupported with good head control. He had
normal power in all muscle groups but hypotonia
with brisk tendon reflexes and negative Babinski
sign. The rest of his examination was negative.
All his laboratory investigations were normal,
including blood and cerebrospinal fluid lactate,
liver function, calcium, magnesium, peroxisomal
address correspondence to:
Dr Maliha A. AL-Bloushi, Department of Pediatrics, Mubarak Al-Kabeer Hospital, Kuwait. Tel: 5318502, Pager: 9174029, E-mail: [email protected]
316
Neuronal Ceroid Lipofuscinoses: Report of Five Cases in Kuwait
December 2006
Fig. 1: H&E stained section shows brownish pigment granules in dermal
fibroblasts (arrows).
Fig. 2: The granules stained positively with sudan black, suggesting a
ceroid-lipofuscin nature (arrows).
function tests, lysosomal enzymes, urine organic
acid and aminoacid chromatography and karyotype.
EEG was moderately abnormal with abnormal
background activity. Electroretinogram (ERG) suggested
a marked disturbance with almost loss of function
in the visual pathways to the cerebral cortex. Visual
evoked potential (VEP) was normal. Brain MRI
showed severe cerebral atrophy with hypointense
thalami and incomplete myelination of the white
matter. His hearing threshold was equivocal in both
ears. The diagnosis of INCL and LINCL were
considered which are caused by deficiency of
palmitoyl protein thioesterase (PPT) and tripeptidyl
amino peptidase I (TPP) respectively. PPT assay
showed low levels of 0.6 nmol/hr/mg ptn (normal
range of 17-139) consistent with the diagnosis of
INCL with normal TPP assay.
He was treated with sodium valproate for his
myoclonic seizures with relatively good control.
The clinical course was of progressive deterioration
and regression. When last seen he was eleven years
old with severe spastic quadriplegia and
contractures at all joints, decorticate posturing and
pendular nystagmus.
Case 4
The fourth case is RS, the product of a full term
delivery. She had uneventful pre, peri and neonatal
periods. Her parents were related and she had one
healthy brother. She was developmentally normal
with no problems till the age of three years when
she, according to the parents, started to lose
milestones: lost speech at three years had deterioration
in motor skills with frequent falls and was unable
to climb stairs at four years. From the age of 4.4
years, she had frequent myoclonic seizures.
We saw her for the first time at the age of five
years. Examination revealed a friendly girl,
interested in her surroundings. There was no
dysmorphism although she had microcephaly, with
weight and height on the 50th centile. Her gait was
spastic. Cranial nerve examination was normal
including both fundi. She had generalized
hypertonia with clonus at the ankles, brisk deep
tendon reflexes and positive Babinski sign. There
was no weakness in any muscle groups, no
neurocutaneous stigmata, normal liver size and no
palpable spleen.
All her laboratory investigations were normal
including blood lactate, blood ammonia, liver
function tests, calcium, magnesium, bicarbonate,
peroxisomal function, lysosomal enzymes, urine
organic acid and aminoacid chromatography
karyotype. EEG was markedly abnormal. Brain
MRI showed cerebral atrophy with hypointense
thalami with incomplete myelination of the white
matter in the occipital region.
Full thickness skin biopsy confirmed the
diagnosis of neuronal ceroid lipofuscinoses. Skin
biopsy specimen was divided into three portions.
One portion was fixed in 3% glutaraldehyde and
processed for electron microscopy. A second
portion was fixed in 10% buffered formalin and
processed routinely for light microscopy. The third
portion was sectioned fresh on a cryostat, mounted
in saline and examined under fluor escence
microscope. H&E stained sections showed
Case 2 and 3
The second and third cases are siblings of case
one, a girl (ten year old now) and a boy (eight year
old) both of whom had similar presentation and
course. The PPT assay was also low in both: 1.9
nmol/hr/mg ptn and 1.1 nmol/hr/mg ptn
respectively. Both mother and father had the
enzyme assay. It was 10.3 nmol/hr/mg ptn in the
former and 20 nmol/hr/mg ptn in the latter
suggestive of carrier state in both parents. All had
normal TPP levels.
The mother became pregnant for the fourth time
in 2002 and chorionic villous sampling (CVS) of her
fetus revealed PPT level of 44 nmol/hr/mg ptn.
She gave birth to a healthy boy who is now two
year old.
December 2006
KUWAIT MEDICAL JOURNAL
317
Fig. 3: The granules demonstrate whitish autofluorescence under the
fluorescence microscope (asterisk).
brownish pigment granules in dermal fibroblasts
(Fig. 1) as well as within sweat gland epithelium.
The granules were negative with stains for melanin
and haemosiderin but stained positively with
sudan black, suggesting a ceroid-lipofuscin nature
(Fig. 2). Electron microscopy showed amorphous
densities and residual bodies (Fig. 3). The granules
also demonstrated whitish autofluorescence under
the fluorescence microscope (Fig. 4). She was
treated with sodium valproate for her epilepsy with
good control of her seizures but there was
progressive deterioration in her motor skills
leading to loss of ability to walk independently.
Case 5
MF is a girl who was born after normal
pregnancy at term to distantly related parents. She
had three healthy siblings. She had acquired
normal skills till the age of seven years when she
had few attacks of generalized tonic clonic seizures
for which she was treated with carbamazepine,
with good control for two years. She presented to
us at nine years of age with progressive speech loss,
change in behavior and interactions and loss of
sphincter control. She became withdrawn and
stopped going to school because of her condition
and worsening seizures.
Examination revealed a wasted child, not
interactive and not interested in her surroundings.
Her head circumference was on the 25th centile,
weight on the 10th centile and height below the third
centile. There was no opthalmoplegia but she was
not fixing or following. Her fundi were normal.
She was unable to sit still. She had rigidity in the
lower limbs more than the upper limbs. There was
ankle contracture and she demonstrated intention
tremor with myoclonia.
She had no neurocutaneous stigmata or
organomegaly. She followed a relentlessly progressive
course involving loss of motor, visual and cognitive
functions. She had difficulty with swallowing and
Fig. 4: Electron microscopy showing amorphous densities and residual
bodies.
was kept on nasogastric feeding. She also developed
recurrent cough probably secondary to aspiration.
She was treated with sodium valproate for her
epilepsy.
All her investigations were normal including
blood and cerebrospinal fluid (CSF) lactate, CSF
routine and titers for chronic infections including
measles, liver function, calcium, magnesium, blood
biotinidase activity, peroxisomal function, lysosomal
enzymes, karyotype, urine organic acid and
aminoacid chromatography and nerve conduction
study. EEG was markedly abnormal but not
suggestive of subacute sclerosing panencephalitis
(SSPE). Brain MRI showed hypointense thalami
with increased signal intensity in the occipital
white matter affecting right more than left. The
diagnosis was confirmed by skin biopsy
demonstrating autoflourescent intracellular material.
DISCUSSION
NCLs are relatively frequent group of inherited
disorders. They occur world-wide with varying
incidence[11]. In Europe the incidence is 1.2-1.6 /
100,000 live births[12]. Cumulative incidence was
1.61 / 100,000 live births but 0.87 / 100,000 for
JNCL and 0.73 for the infantile NCL[12]. The highest
reported incidence is in Finland (1:20,000 live
birth)[11].
Common to all NCLs is lysosomal accumulation
of autoflourescent ceroid lipopigment material in
neural and extraneural cells [1,9]. The autoflourescent
318
Neuronal Ceroid Lipofuscinoses: Report of Five Cases in Kuwait
December 2006
Table 1: Characterestics of the major neuronal ceroid lipofuscinoses [5]
Range
Onset
(Yr)
Mean
Onset
(Yr)
Juvenile
4-9
5.93 ± 1.35
Late infantile/
early childhood
Infantile
1-3
2.54 ± 0.71
0 - 1.5
Adult
27 - 28
Atypical
Variable
First
Symptom
Visual,
behavioral
Seizures
0.96 ± 0.50 Deterioration
myoclonus
29.67 ± 4.80 Seizures/
motor
Variable
Variable
Course
Incidence
EM
(% Neuronal
PredoOnset to
Ceroidminant
Death Lipofucinoses) Findings
Genetics
Chromosome
Chronic
16
49
FP
AR
D16
Acute
6
21
CL
AR
Not D16
Acute
4
9
GR
AR
DI
Chronic
> 20
9
GR
AR/AD
UNK
Variable
> 20
12
Variable
Unknown
Unknown
FP = Fingerprint cytosomes; CL = curvilinear cytosomes; GR = granular cytosomes; AR = autosomal recessive; AD = autosomal dominant; UNK = unknown genetics; D =
chromosome
intracellular lipopigment tend to distend the
cytoplasm of affected cells. Despite the multisystem
distribution, only brain tissue shows severe
dysfunction and cell death[4,5]. It is now known that
ceroid and lipofuscin are composed of many
different substances, including lipids, waxy
pigments and a variety of proteins[5].
The cytosomes consists of mixtures of four
distinct and characteristic membrane-bound
osmiophilic profiles; classic lipofuscin, fingerprint
profiles which predominate in chronic juvenile
form, curvilinear inclusion bodies in infantile forms
and pure granular profiles which predominate in
some infantile and in late adult type[5].
The disorder is characterized by visual
impairment, progressive myoclonic epilepsy,
cognitive decline and premature death[1,7, 8]. The
course reflects progressive neurodegeneration.
Eventually every patient shows psychomotor
deterioration. The outcome is always lethal within
a few years[13]. Retinal degeneration is an early
consequence[14,15]. The electroretinogram (ERG) is
abnormal early in all three types of childhood NCL
and eventually is totally ablated[14,16].
The NCLs are subdivided into several subtypes
(Table 1) according to age of onset, clinical course
and ultrastructural features of the storage material.
The three main childhood varieties include infantile
NCL (INCL) or (CLN1), late-infantile NCL ( LINCL)
or (CLN2) and juvenile NCL (JNCL) or (CLN3)[8,17].
Molecular genetics of these three subtypes was
recently clarified.
In the first subtype, INCL, or Santavuori - Haltia
- Hagberg disease, there are mutations in genes
encoding a lysosomal enzyme, palmitoyl protein
thioesterase 1(PPT1) with locus CLN1 on
chromosome 1p32[18]. This type is associated with
predominance of granular inclusions in biopsied
material. Cases 1-3 in this study represent this
subtype based on demonstration of low PPT levels
in the subjects and borderline levels in both parents
making them obligate carriers. Mutations in CLN1
gene also result in different childhood phenotypes
(LINCL and JNCL) with granular osmiophilic
deposits[18,19]. In addition to childhood forms,
mutations in this gene also result in NCL in adults
with onset in the fourth decade [20]. All CLN1
patients are deficient in PPT1. Similar to childhood
forms with granular osmiophilic deposits, few
cases were reported in a ANCL with autosomal
dominant inheritance (Parry type) but interestingly
with normal PPT1 enzyme level probably indicating
gene distinct from CLN1-CLN8 genes [21].
The second subtype, LINCL, or JanskyBielschowsky disease, is caused by mutations in
CLN2 gene which encodes a lysosomal enzyme
tripeptidyl peptidase 1 (TPP1) with locus on
chromosome 11p15[2,18]. The fourth case is an
example of this subtype based on the age of
presentation and characteristic inclusions seen in
the skin biopsy.
The third subtype, JNCL or Batten disease, is
caused by mutations in gene encoding a 438aminoacid membrane protein (CLN3 on
chromosome 16p12.1) commonly related to 1.02kb
deletion[5,18]. There is predominance of curvilinear
inclusion bodies in biopsied material. This is
represented by our fifth case. As in this case, it is
characterized clinically by visual and behavioral
problems with slow progression over a few years [5].
The mean age of onset is 5.93 ± 1.35 years with
onset between four and nine years. In contrast to
our case, seizures occur later in life. Usually, the
initial symptom is visual deterioration but in our
case speech loss was the initial concern. It is
possible that visual problems were not noted
initially or were overshadowed by more obvious
symptoms of speech loss and impaired interaction.
Other childhood forms include Finnish variant
LINCL (CLN5) with locus on chromosome 15q21-
December 2006
KUWAIT MEDICAL JOURNAL
23[18] and Northern epilepsy or progressive epilepsy
with mental retardation (CLN8)[22]. A total of 114
mutations have been described in the five human
genes which cause NCL [23].
Early diagnosis is mandatory for avoiding
further cases in families with hereditary metabolic
brain disorders[24]. Diagnosis is made on the basis of
clinical, electrophysiological, radiological and
pathologic examination including electron
microscopy[6]. Although only biochemical and
molecular gentetic studies allow for definitive
diagnosis, ultrastructural studies of biopsy material
are still very useful [2].
Numerous tissues and organs are available for
biopsy, among them brain (historical), rectum,
skeletal muscle and peripheral nerve (largely by
coincidence), skin and conjunctiva (the latter
inferior to former in diagnostic yield) [10].
Unfortunately, the most convenient diagnostic
method of examining circulating lymphocytes was
not done. Treatment includes supportive measures
and anticonvulsant medication.
Neuropathologic and neuroradiologic explanation
of clinical symptomatology correlates best with
neuronal loss and not neuronal storage[25]. This
neuronal loss especially of dopaminergic neurons
makes patients with JNCL and ANCL more
susceptible to develop a life-threatening condition,
neuroleptic malignant syndrome, after exposure to
antipsychotic therapy. It should be considered
when these patients develop hyperthermia,
autonomic instability, extrapyramidal symptoms
with or without altered level of consciousness. A
high index of suspicion with early intervention is
vital to avoid lethal outcome of neuroleptic
malignant syndrome[26-28].
Early diagnosis is important for genetic
counseling. Delay in diagnosis could be avoided by
high index of suspicion in patients with
unexplained visual loss, careful examination of
lymphocytes for vacuolation and inclusion bodies
together with molecular genetics studies. If our first
case was diagnosed early in the course, genetic
counseling and perinatal diagnosis would have
helped the family to avoid having further cases.
Whether this is a true statement or not, is to be
debated as abortion is generally prohibited in
Islamic culture with only few exceptions. However,
the first family in this study did resort to this
option.
REFERENCES
1.
2.
Weimer JM, Kriscenski-Perry E, Elshatory Y, Pearce DA.
The Neuronal ceroid lipofuscinoses: mutations in different
proteins result in similar disease. Neuromolecular Med
2002; 1:111-124.
Wisniewski KE , Kida E, Golabek AA, Kaczmarski W ,
3.
4.
5.
6.
7.
8.
9.
10.
11.
12.
13.
14.
15.
16.
17.
18.
19.
20.
21.
22.
23.
24.
319
Connel F, Zhong N. Neuronal ceroid lipofuscinoses:
classification and diagnosis. Adv Genet 2001; 45:1-34.
Mitchison HM, Mole SE. Neurodegenerative disease: The
neuronal ceroid lipofuscinoses (Batten disease). Curr Opin
Neurol 2001; 14:795-803.
Kida E, Golabek AA, Wisniewski KE. Cellular pathology
and pathogenic aspects of Neuronal ceroid lipofuscinoses .
Adv Genet 2001; 45:35-68.
Dyken PR. Neuronal ceroid-lipofuscinoses. Pediatrics
Neurology, Principles and Practice, 1999:839-846.
Zong N. Neuronal ceroid lipofuscinoses and possible
pathogenic mechanism. Mol Genet Metab 2000; 71:195-206.
Peltonen L, Savukoski M, Vesa J. Genetics of the neuronal
ceroid lipofuscinoses. Curr Opin Genet Dev 2000; 10:299305.
Goebel HH. The neuronal ceroid-lipofuscinoses. Semin
Pediatr Neurol 1996; 3:270-278.
Sondhi D, Hackett NR, Apblett RL, Kaminsky SM,
Pergolizzi RG, Crystal RG. Feasiblilty of gene therapy for
late neuronal ceroid lipofuscinosis. Arch Neurol 2001;
58:1793-1798.
Goebel HH. Morphologic diagnosis in Neuronal ceroid
lipofuscinosis. Neuropediatrics 1997; 28:67-69.
Santavuori P, Lauronen L, Kirveskari E , Aberg L, Sainio
K, Autti T. Neuronal ceroid lipofuscinoses in childhood.
Neurol Sci 2000; 21:35-41.
Crow YJ, Tolmie JL, Howatson AG , Patrick WJ, Stepenson
JB. Batten disease in the west of Scotland 1974-1995
including five cases of the juvenile form with granular
osmiophilic deposits. Neuropediatrics 1997; 28:140-144.
Jongen PJ, Gabreels FJ, Stekhoven JH, Renier WO, Le
Coultere R, Begeer JH. Early infantile form of neuronal
ceroid lipofuscinosis. Four Dutch cases and review of the
literature. Clin Neurol Neurosurg 1987; 89:161-167.
Wilkinson ME. Ceroid lipofuscinosis, neuronal 3, JuvenileBatten disease: case report and literature review. Optometry
2001; 72:724-728.
Birch DG. Retinal degeneration in retinitis pigmentosa and
neuronal ceroid lipofuscinosis: An overview. Mol Genet
Metab 1999; 66:356-366.
Weleber RG. The dystrophic retina in multisystem
disorders:the electroretinogram in neuronal ceroid
lipofuscinoses. Eye 1998; 12:580-590.
Gardiner RM. Genetic analysis of Batten disease. J Inherit
Metab Dis 1993; 16:787-790.
Mole S, Gardiner M. Molecular genetics of the Neuronal
ceroid lipofuscinoses. Epilepsia 1999; 40:29-32.
Wisniewski KE, Kida E, Connel F, Zhong N. Neuronal
ceroid lipofuscinoses research update. Neurol Sci 2000;
21:S49-56.
Van Digglen OP, Thobois S, Tilikete C, et al. Adult Neuronal
Ceroid Lipofuscinosis with Palmitoyl-Protein Thioesterase
Deficiency: First adult-onset patients of a childhood
disesase. Ann Neurol 2001; 50:269-272.
Nijssen PC, Ceuterick C, van Diggelen OP, et al. Autosomal
dominant adult neuronal ceroid lipofuscinosis: a novel form
of NCL with granular osmiophilic deposits without
palmitoyl protein thioesterase 1 deficiency. Brain Pathol
2003; 13:574-581.
Ranta S, Lehesjoki AE. Northern epilepsy, a new member
of the NCLfamily. Neurol Sci 2000; 21:S43-47.
Mole SE, Zhong NA, Sarpong A, et al. New mutations in the
neuronal ceroid lipofuscinosis genes. Eur J Paediatr Neurol
2001; 5:7-10.
Santavuori P, Vanhanen SL, Autti T. Clinical and
neuroradiological diagnostic aspects of neuronal ceroid
lipofuscinoses disorders. Eur J Paediatr Neurol 2001; 5:157161.
320
Neuronal Ceroid Lipofuscinoses: Report of Five Cases in Kuwait
25. Boustany RM. Neurology of neuronal ceroid- lipofuscinoses:
late infantile and juvenile types. Am J Med Genet 1992;
42:533-535.
26. Vercammen L, Buyse GM, Proost JE, et al. Neuroleptic
malignant syndrome in juvenile neuronal ceroid
lipofuscinosis associated with low-dose risperidone
December 2006
therapy. J Inherit Metab Dis 2003; 26:611-612.
27. Refi A, Schneider MF, Hoyer A, et al. Neuroleptic malignant
syndrome in Kufs’ disease. J Neurol Neurosurg Psychiatry
2003; 74:385-387.
28. Gupta S, Nihalani ND. Neuroleptic Malignant Syndrome.
Prima Care Companion J Clin Psychiatry 2004; 6:191-104.
December 2006
KUWAIT MEDICAL JOURNAL
Case Report
Adrenal Carcinoma with Cardiac Metastasis in a Child:
Case Report
Abdelmohsen Ben-Nakhi, Ali Hussain, Khaledah Dashti
Department of Radiology, Mubarak Al-Kabeer Hospital, Ministry of Public Health, Kuwait
Kuwait Medical Journal 2006, 38 (4): 321-323
ABSTRACT
Adrenal carcinoma is very rare in children, and cardiac
metastasis from this tumor is even rarer. We present such
a case and discuss its management. A ten year old boy
presenting with hirsutism was referred to the radiology
department of Mubarak Al-Kabeer Hospital for
investigation. The investigations performed included US
of the abdomen and CT examination of the chest and
abdomen. In addition, the patient also had hormonal and
routine biochemical investigations. The Ultrasound and
CT examinations revealed a solid mass arising from the
right adrenal gland, infiltrating into the inferior vena
cava and extending into the right atrium. Ultrasound
guided fine needle aspiration of the mass, confirmed the
diagnosis of adrenal carcinoma. The case is reported
because of its rare nature.
KEYWORDS: adrenal carcinoma, cardiac metastasis, imaging
INTRODUCTION
Adrenocortical carcinoma is a rare malignancy
in childhood[1, 2] . Extension of this tumor through
the IVC into the right atrium is even rarer. The
estimated incidence of this tumor is about 1 in 1,
700,000[1]. There are limited reports of cases with
extension into the IVC and the right atrium. To our
knowledge only ten such cases have been
previously reported including one case with a
tumor in the left adrenal gland[3]. We report the case
of a ten year old boy with a right adrenocortical
carcinoma, extending into the IVC and the right
atrium. To our knowledge this is the first case
report from the middle east region.
CASE REPORT
A ten-year-old Omani boy presented in January
2001 with a three month history of weight gain and
edema of both lower limbs in addition to features of
precocious puberty (facial, axillary and pubic hair)
for two years.
Physical examination revealed a short-statured
and grossly overweight child with signs of precocious
puberty. The genitalia appeared small and an
adequate examination was not possible because of
gross obesity. Examination of the cardio-vascular
system at the time of admission revealed raised BP
(165/95) and pansystolic murmur over the
tricuspid area. On abdominal examination an ill
defined mass was palpable in the right hypochondrium
extending to the right lumbar region.
Hormonal study revealed that testosterone (47
nmol/l), 17 OH progesterone (21 nmol/l), DHEAS
(45 nmol/l) and androstendione (14 nmol/l) were all
raised. The serum biochemistry, liver and renal
functions were unremarkable.
Ultrasound examination of the abdomen showed
a large solid mass arising from the right adrenal
gland measuring 12 cm in diameter, infiltrating into
the IVC (Fig 1a) and extending into the right atrium
(Fig 1b). CT scan of the chest and abdomen was
done for further workup. It confirmed the right
adrenal mass (Fig 2a) extending into the IVC (Fig
2b) and the right atrium (Fig 2c). The lungs were
clear and there was no evidence of bone metastasis
of the scanned bones.
The intracardiac extension of the mass was also
confirmed on echocardiogram.
Ultrasound guided fine needle aspiration
biopsy confirmed adrenocortical carcinoma.
The child’s parents refused any treatment and
got discharged against medical advice.
The child was readmitted two weeks later with
acute cardiac failure and died on the third day of
admission.
DISCUSSION
Adrenal cortical carcinoma is a rare tumor in
children comprising only 0.2 % of all childhood
malignant tumors. It often presents with a large
Address correspondence to:
Dr. Abdelmohsen Ben-Nakhi, Department of Radiology, Mubarak Al-Kabeer Hospital, P.O. Box 43787, Code-32052 Hawally, Kuwait. Tel: +965
5336856, Mobile: +965 6322229, Fax: + 965 5618866, E-mail: [email protected]
322
Adrenal Carcinoma With Cardiac Metastasis in a Child: Case Report
Fig 1a
December 2006
Fig 1b
Fig 1: Ultrasound examination showing large tumor thrombus in the IVC (a) [arrows] extending into the right atrium (b)
Fig 2a
Fig 2c
Fig. 2: CT scan of upper abdomen showing the large adrenal mass
infiltrating into the IVC (a & b [arrow heads]) and extending into the right
atrium (c) [arrows]
Fig 2b
abdominal mass and signs of precocious puberty[1].
Despite its often dramatic presentation, there
typically is long delay between the onset of
symptoms and the time of diagnosis.
The clinical features of the tumor include those
caused by the local mass effect, such as flank pain
and abdominal fullness and of those caused by
unregulated hormone production by the tumor[4].
With cortical over production signs and symptoms
of Cushing’s syndrome are noted. Androgen
secretion, which is less common, results in
virilization, hirsutism and amenorrhea. The clinical
features of right atrial involvement are due to
central pulmonary embolization and cardiac and /
or valve obstruction, often with associated congestive
heart failure.
Ultrasound, CT and MRI studies are the main
and effective imaging investigations in assessing
the local as well as the IVC and intracardiac
extension of the tumor[5]. MRI is shown to be the
December 2006
KUWAIT MEDICAL JOURNAL
most sensitive method of diagnosing virilising
adrenocortical tumors in children[6]. The use of Ga67 scintigraphy in detecting tumor recurrence and
in assessing response to therapy has been
reported[1].
Due to the delay in diagnosis, adrenocortical
carcinoma is a fatal disease with poor prognosis.
Complete surgical resection is the only treatment
that offers potentially long term disease free
survival[4]. Chemotherapy with Ortho Para DDD is
recommended for treatment of residual or recurrent
tumor after surgery or for patients with metastatic
disease.
The mean survival without treatment is
approximately three months and with treatment
the five years survival is about 30%. The poor
prognosis is mainly due to the long delay between
the symptoms and the time of diagnosis.
In conclusion, it is imperative that the physician
performs cardiovascular examination in suspected
323
or proven cases of adrenal carcinoma and recognize
the endocrine manifestations of the tumor for
prompt treatment.
REFERENCES
1.
2.
3.
4.
5.
6.
Giles RH, Pozza LD, Uren R. Ga-67 scintigraphy in a child
with adrenocortical carcinoma. Clinical Nuclear Medicine
1993; 18:642-645.
Zderic SA. Renal and adrenal tumors in children. Urol Clin
North Am 2004; 31:607-617.
Lee JJ, Kupfer J, Raissi S, Geller SA and Siegel RJ. Rapid
Extension of left adrenocortical carcinoma into the right
atrium. Journal of American Society of Echocardiography
1998; 11:86-88.
Dunnick NR. Adrenal Carcinoma. Radiology Clinic North
Am 1995; 32:99-108.
Ribeiro J, Ribeiro RC, Fletcher BD. Imaging findings in
pediatric adrenocortical carcinoma. Pediatr Radiol 2000;
30:45-51.
Bonfig W, Bittmann I, Bechtold S, Kammer B, Noelle V,
Arleth S, Raile K, Schwarz HP. Virilising adrenocortical
tumours in children. Eur J Pediatr 2003; 162:623-628.
KUWAIT MEDICAL JOURNAL
December 2006
Case Report
Excision of Ventricular Cysts of Larynx using Zero Degree
and 30 Degree Endoscope
Pradeep Shenoy, Sohail Abdul Malik, Rashid Al Duwillah,
Department of Otorhinolaryngology, Armed Forces Hospital, Kuwait
Kuwait Medical Journal 2006, 38 (4): 324-325
ABSTRACT
A case of ventricular cyst of larynx has been described,
where 0º and 30º nasoendoscope was used to get good
access and complete excision. Clinical presentation and
treatment of ventricular cyst of larynx in literature has
been discussed. Though these are rare they could present
as an emergency at any age.
KEY WORDS: deroofing, marsupialization, unroofed, ventricular cyst of larynx, 0º and 30º rigid nasoendoscope
CASE REPORT
A 23-year-old male patient attended the ENT
clinic with dysphonea, muffled voice and painful
swelling in the left side of the neck for the past three
days. Indirect laryngoscopy revealed pooling of saliva
and a globular cystic swelling in the left ventricle.
Neck examination unveiled a diffuse swelling in
the left anterior triangle. After 48 hours of
intravenous antibiotics and steroids, the ventricular
and neck swelling was more localized. It was
confirmed by X - ray (Fig. 1) and CT scan of neck
(Fig. 2). CT scan of the neck showed a well-defined
peripherally enhancing cystic lesion in the
supraglottic compartment of the larynx measuring
3.6 x 3 x 1.7 cm in size and it was arising from the
left ventricle, extending into the lumen medially
and paraglottic space laterally through the
thyrohyoid membrane.
Fiberoptically guided nasoendotracheal intubation
was done. Boyle-Davis gag with a long tongue
blade was used to get good exposure and the cyst
was decapped using 0º and 30º Hopkins
nasoendoscope (Fig. 3). The raw area after unroofing
was cauterized (Fig. 4).
Postoperative period was uneventful. The
patient was discharged after 48 hours with no
further recurrence.
DISCUSSION
Laryngeal ventricle cysts are rare and less
common in the pediatric population than in
adults[1]. Congenital laryngeal cyst has an incidence
of 1.82 per 100,000 live births[2]. Congenital cysts are
asymptomatic unless they are large enough to
cause stridor and respiratory obstruction in infants
and children[3].
The most common symptoms of a laryngeal cyst
are hoarseness, local foreign body sensation and
dysphonea[4]. Small cysts are not obvious at
endoscopy and are indeed buried below the mucosa
in soft tissues[5]. Flexible fiberoptic laryngoscopy
could help to detect medium and large cysts[2]. CT
scan proved useful for intralaryngeal location and
planning of the surgical excision[6].
Small and medium sized cysts are excised using
carbondioxide laser[7] or cup forceps[5]. Endoscope
deroofing is as effective as endoscopic excision but
is technically simpler and thus is recommended as
the treatment of choice[2]. Recurrence rate is higher
after endoscopic marsupialization procedures[8].
Repeated needle aspiration of the cyst failed to
provide sustained clinical improvement[6]. Laryngeal
cysts, when they are large and becomes extra
laryngeal by piercing the thyrohyoid membrane are
excised by paramedian or laryngofissure approach[3].
CONCLUSION
We have reported and discussed the clinical
presentation of a ventricular cyst in an adult. Rigid
Hopkins fiberoptic nasoendoscope (0º and 30º) was
used to access the cyst and complete its excision.
ACKNOWLEDGEMENT
Our special thanks to Colonel Ali Ahmed Essa,
Director of Armed Forces Hospital, Kuwait for his
kind permission to present this case study and to
Mr C M Khan, Medical Secretary for his secretarial
assistance.
Address correspondence to:
Dr. Pradeep Shenoy, DLO, FRCS, Post Box No. 8728, 22058 - Salmiya, Kuwait. Tel: 5623257 (Res), 9756935 (Mobile), Fax: +965 - 5623257, Email: [email protected]
December 2006
KUWAIT MEDICAL JOURNAL
Fig. 1: Plain X-ray of the ventricular cyst
Fig. 2: CT Scan of ventricular cyst
Fig. 3: Endoscopic view of ventricular cyst
Fig. 4: Endoscopic view after unroofing and cautry
REFERENCES
5.
1.
2.
3.
4.
Civantos FJ, Holinger LD. Laryngoceles and saccular cysts
in infants and children. Arch Otolaryngol Head Neck Surg
1992; 118:296-300.
Pak MW, Woo JK, Van Hasselt CA, et al. Congenital
laryngeal cysts: Current approach to management. J
Laryngol Otol 1996; 110:856-858.
Forte V, Warshawski J, Thorner P, et al. Unusual laryngeal
cysts in the newborn. Int J Pediatr Otorhinolaryngol 1996;
37:261-267.
Newman BH, Taxy TB, Laker HI, et al . Laryngeal cysts in
adults: A clinicopathologic study of 20 cases. Am J Clin
Pathol 1984; 81:715-720.
6.
7.
8.
325
Torium DM, Miller DR, Holinger LD. Acquired subglottic
cysts in premature infants. International Journal of
Paediatric Otolaryngology 1987; 14:151-160.
Ostfield E, Hazan I, Rabinson S, et al. Surgical management
of congenital supraglottic lateral saccular cysts.
International Journal of Paediatric Otorhinolaryngology
1990; 19:289-294.
Martinez Devesa P, Gherfoor K, Lioyd S, et al. Endoscopic
CO2 Laser management of laryngocele. Laryngoscope 2002;
112:1426-1430.
Hogikyan ND, Bastian RW. Endoscopic CO2 Laser excision
of large or recurrent laryngeal saccular cysts in adults.
Laryngoscope 1997; 107:260-265.
326
KUWAIT MEDICAL JOURNAL
December 2006
Case Report
Sickle Cell Intra-Hepatic Cholestasis : A Rare but Fatal
Disease
Saad Al-Zanki, Moza Al-Saleh
Department of Medicine, Al-Amiri Hospital, Kuwait
Kuwait Medical Journal 2006, 38 (4): 326-328
ABSTRACT
Sickle cell intra-hepatic cholestasis is a rare but
potentially fatal complication of sickle cell disease. It is
characterized by fever, jaundice, tender hepatomegaly,
coagulopathy and acute liver failure. Early identification
is essential and the only effective treatment reported is
exchange transfusions. We describe one Hemoglobin SS
patient and review the literature.
KEYWORDS: exchange transfusions, jaundice, sickle cell intra-hepatic cholestasis,
INTRODUCTION
In clinical studies, it was noted that there is an
association between sickle cell disease and hepatic
dysfunction[1-5].These dysfunctions occur mainly in
patients with homozygous sickle cell anemia but to
a lesser extent in patients with sickle cell trait, sickle
C disease and hemoglobin S B-thalassemia. One of
the rare but potentially fatal complications of sickle
cell anemia is known as sickle cell intra-hepatic
cholestasis, a clinical syndrome thought to represent
a severe form of hepatic crisis[3]. Sickle cell intrahepatic cholestasis is characterized by the acute
onset of hepatomegaly, extreme hyperbilirubinemia
with a level of 273 mg/dl (around 4600 µmol/l)
documented in one patient[6], coagulopathy and
acute liver failure[4,7].
Recent reports have described reversal of this
process within 48 hours in seven patients with
vigorous exchange transfusions and correction of
coagulopathy with fresh frozen plasma [6,8-12].
We describe one patient with sickle cell anemia
with recurrent admissions due to fever, jaundice,
leukocytosis, coagulopathy and extreme hyperbilirubinemia. We also describe the types of hepatic
injuries and clinical syndromes found in sickle cell
anemia patients with particular attention to sickle
cell intra-hepatic cholestasis.
CASE REPORT
Mr HN is a 22-year-old Kuwaiti male studying
Dentistry in Egypt and who is known to have sickle
cell disease. He presented to the medical department
complaining of fever and generalized body aches
for two days accompanied by jaundice. He
informed that jaundice was on and off for the last
Address correspondence to:
Dr.Saad AL-Zanki, Mishref
[email protected]
two years and was associated with intermittent
episodes of itching and dark urine. This was on a
background history of intermittent right upper
quadrant pain, anorexia and weight loss of six
kilograms over the last two months. There was no
history of nausea, vomiting, bleeding or change in
bowel habits.
He stated that he was admitted once at the age
of six years for an exchange transfusion, but he
denie any previous admissions with vaso-occlusive
crises.
He was on ibuprofen and mefenamic acid for
pain and on phenobarbitone for itching.
On physical examination, he was febrile and
deeply jaundiced with a pulse rate of 90 per minute
(regular) and a blood pressure of 110/70 mmHg.
He had no stigmata of chronic liver disease and no
hepatic flab.
Abdominal examination revealed a tender
upper abdomen with a hepatomegaly of 3 cm
below the costal margin. Other systems examination
was unremarkable. His initial investigations
showed the following; FBC: Hb 114 g/l; MCV 104.2
fl (80-96 fl); WBC 15.7 x 109 /l; Platelets 223 x 10 9 /l
and Reticulocyte count of 5.7 %. LFT showed total
bilirubin 417 µmol/l; direct bilirubin 236.3 µmol/l;
ALT 329 IU/l; AST 826 IU/l; LDH 1248 IU/l; ALP
625 IU/l; Amylase 324 IU/l.
Urine routine and microscopy revealed trace
proteins; +urobilinogen; +bilirubin; +erythrocytes.
Serum urea and electrolytes were normal. An
abdominal ultrasound was normal apart from one
single large stone in the gallbladder with no CBD
dilatation.
P.O.Box 1813, Zip code 40169, Kuwait. Tel: +965- 53882376, Mob: +965- 9852353, E-mail:
December 2006
KUWAIT MEDICAL JOURNAL
Fig 1: Liver biopsy showing early fine fibrosis (top arrow) and
bile duct proliferation (bottom arrow) [H&E x 300]
HN was admitted to the medical ward where i.v.
fluids, cefotaxime and metronidazole were
initiated. The next morning, an urgent ERCP was
done which was found to be normal apart from the
single large gallbladder stone. Later, the hematologist
and hepatologist were consulted. Our hematologist
advised for exchange transfusion and the
hepatologist asked for the following investigations:
Ceruloplasmin: normal. Ferritin 1185.9 µg/l (20260 µg/l); IgA6.22 g/l (0.8-4 g/l); IgG 17.2 g/l (7-18
g/l); IgM 0.82 g/l (0.4-2.5 g/l). ANA, AMA, LKM,
ASM and reticulin were negative.
Virology screening: Hep BsAg (negative); Anti
HCV (negative); HIV test (negative)
Hemoglobin electrophoresis post first exchange
transfusion showed: HbF 3%, HbS 35%, HbA2 2.2%.
Four days later, the condition of the patient
improved and all cultures were found to be
negative. On the seventh day, the patient was
discharged home and his liver function tests on
discharge were as follows:
Total bilirubin 415 µmol/l; direct bilirubin 271.4
µmol/l; ALT 55 IU/l; AST 187 IU/l; ALP 103 IU/l.
Ten days post discharge, the patient was readmitted with fever, deep jaundice and right upper
quadrant pain. Serum biochemical findings
included AST/ALT 157/56 IU/l; total bilirubin 593
µmol/l; direct bilirubin 374 µmol/l; ALP 99 IU/l;
Reticulocyte count was 7.22%; LDH was not done.
Next day, a liver biopsy was done and showed:
bile plugs in some bile ducts; moderately expanded
portal tracts with edema; bile duct proliferation
(Fig.1); early fine fibrosis (Fig.1); sickled cells in
sinusoids (Fig. 2); areas of peliosis hepatic; mild
siderosis in kupffer cells. These histologic findings
are consistent with a major bile duct obstruction;
therefore, a second ultrasound abdomen was done
which showed mild common bile duct dilatation of
six mm with mild intra-hepatic dilatation. It was
followed by a second ERCP which was the same as
the first one and papillotomy was done. Post-
327
Fig 2: Liver biopsy showing sickled cells in sinusoids (arrows) [H&E x 300]
procedure, the patient had worsening of his liver
function biochemistry and was discharged against
medical advice.
Three weeks later, the patient was admitted
again with abdominal pain, nausea and vomiting.
His liver function test showed; total bilirubin 433
µmol/l; direct bilirubin 213 µmol/l; ALT 33 IU/l;
AST 127 IU/l; ALP 158 IU/l. The patient agreed for
a second exchange transfusion (40 days after the
first one) and liver function biochemistry showed ;
total bilirubin 342 µmol/l; direct bilirubin 164
µmol/L; ALT 22 IU/l; AST 99 IU/l; ALP 102 IU/l.
Ten days later, a third exchange transfusion was
done with a liver biochemistry post transfusion
showing; total bilirubin 192 µmol/l; direct bilirubin
95 µmol/l; ALT 34 IU/l; AST 137 IU/l; ALP 127
IU/l. Later, the patient decided to travel to the UK
for continuation of his treatment. On discharge, his
HbS was 18%. Patient expired two months later.
DISCUSSION
Hepatic injuries in sickle cell disease most
commonly occur due to multiple transfusions
secondary to iron overload, or acute/chronic
hepatitis C. It can also occur as a complication of
chronic hemolysis, like the development of
pigment stones with consequent cholecystitis or
choledocholithiasis.
Furthermore but less common, hepatic injury
can be directly related to the sickling process and
hence the term most often used to describe these
syndromes is sickle cell hepatopathy e.g., acute
hepatic crisis and hepatic sequestration crisis.
Sickle cell intra-hepatic cholestasis is a rare form
of sickle cell hepatopathy. It is potentially fatal with
a poor prognosis[3,13-16]. Therefore, early identification
is essential. It is thought to represent a severe form
of hepatic crisis [3].
The presentation is similar to acute sickle
hepatic crisis with fever, right upper quadrant pain,
nausea, vomiting, tender hepatomegaly and a
328
Sickle Cell Intra-Hepatic Cholestasis : A Rare but Fatal Disease
striking jaundice. Sheehy[3] described this syndrome
as a very severe form of hepatic crisis marked by
sudden onset of severe right upper quadrant pain,
progressive hepatomegaly, coagulopathy with
hemorrhage and extreme hyperbilirubinemia.
In one case report, bilirubin level reached 273
mg/dl[6] (around 4600 µmol/l). This is caused by a
combination of ongoing hemolysis, intra-hepatic
cholestasis and renal impairment.
Despite its fatality, we were able to find reports
describing seven patients who did survive with
vigorous exchange transfusions and correction of
coagulopathy with fresh frozen plasma [6,8-12].
Shao and Orringer[9] have described two cases of
sickle cell intra-hepatic cholestasis with similar
presentations, but in which very different therapeutic
approaches led to very different clinical outcomes.
The first patient presented with jaundice, right
upper quadrant pain, nausea, fever and leukocytosis.
Ultrasound abdomen showed multiple gallbladder
stones with no ductal dilatation. The decision was
made to perform a cholecystectomy for him. The
procedure went well with no complications but
eleven days later the patient expired.
The second patient had similar clinical features
and even worse blood chemistry. His surgery was
cancelled and the decision was made to perform
exchange transfusions using packed red blood cells
and fresh frozen plasma. Post exchange transfusion,
all his hematological parameters improved and he
underwent an uneventful cholecystectomy six
weeks later.
They concluded that early identification of this
clinical syndrome is essential, as exchange
transfusions with both packed red blood cells and
fresh frozen plasma can often correct the
coagulopathy. They also suggested that any type of
surgical intervention is best deferred until the
patient has had sufficient time to recover from the
acute illness.
In our patient, sickle cell intra-hepatic
cholestasis was not the first in our list of differential
diagnosis, first due to its rarity, and secondly due to
the fact that this patient had a fairly uncomplicated
sickle cell anemia over twenty two years of his life,
with no history of vaso-occlusive crisis or regular
exchange transfusions.
Once the diagnosis had been made and
exchange transfusions started, the patient’s condition
along with his liver function biochemistry
improved dramatically.
In summary, we have reported a case of sickle
cell intra-hepatic cholestasis. Whereas the
presenting manifestations include fever, right
upper quadrant pain, tender hepatomegaly and
leukocytosis, the most striking clinical feature is
extreme hyperbilirubinemia.
December 2006
Awareness and early recognition of this
potentially fatal condition is important, as
exchange transfusions can often reverse the process
of intra-hepatic cholestasis and can be life saving.
ACKNOWLEDGMENT
We thank all our friends and colleagues in Dr S
Narayanan’s unit in Amiri Hospital, Kuwait for
their support. We would also offer special thanks to
Dr S Narayanan, consultant physician, Dr John
Patrick Madda, consultant pathologist and Dr
Amal Khamis, consultant hematologist for their
time, effort and advise in the preparation of this
report.
REFERENCES
1.
2.
3.
4.
5.
6.
7.
8.
9.
10.
11.
12.
13.
14.
15.
16.
Bauer TW, Moore GW, Hutchins GM. The liver in sickle cell
disease. A clinicopathologic study of 70 patients. Am J Med
1980; 69:833-837.
Jonson CS, Omata M, Tong MJ, Simmons JF Jr., Weiner J,
Tatter D. Liver involvement in sickle cell disease. Medicine
1985; 64:349-356.
Sheehy TW. Sickle cell hepatopathy. South Med J 1977;
70:533-538.
Schbert TT. Hepatobiliary system in sickle cell disease.
Gastroenterology 1986; 90:2013-2021.
Rosenblate HJ, Eisenstein R, Holmes AW. The liver in sickle
cell anemia.A clinical-pathologic study. Arch Pathol 1970;
90:235-245.
Stephan JL, Merpit-Gonon E, Richard O, Raynaud-Ravni C,
Freycon F. Fulminant liver failure in a 12-year-old girl with
sickle cell anemia: favourable outcome after exchange
transfusions. Eur J Pediatr 1995; 154:469-471.
Serjeant GR. The liver. In: Sickle cell disease. Oxford,
England: Oxford University Press; 1985, p 101-108.
Sheehy TW, Law DE, Wade BH. Exchange transfusion for
sickle cell intrahepatic cholestasis. Arch Intern Med 1980;
140:1364-1366.
Shao SH, Orringer EP. Sickle cell intrahepatic cholestasis:
approach to a difficult problem. Am J Gastroenterol 1995;
90:2048-2050.
Svarch E, Gonzalez A, Villaescusa R, Basanta P. Plasma
exchange for acute cholestasis in homozygous sickle cell
disease. Haematologia 1986; 9:49-51.
Morrow JD, McKenzie SW. Survival after intrahepatic
cholestasis associated with sickle cell disease. J Tenn Med
Assoc 1986; 79:199-200.
Betrosian A, Balla M, Kafiri G, Palamarou C, Sevastos N.
Reversal of liver failure in sickle cell vaso-occlusive crisis.
Am J Med Sci 1996; 311:292-295.
Green TW, Conley CL, Berthrong M. The liver in sickle cell
anemia. Bull J Hopkins Hosp 1953; 92:99-122.
Song YS. Hepatic lesions in sickle cell anemia. Am J Pathol
1957; 33:331-344.
Klion FM, Weiner MJ, Schaffner F. Cholestasis in sickle cell
anemia. Am J Med 1964; 37:829-832.
Owen DM, Aldridge JE, Thompson RB. An unusual hepatic
sequela of sickle cell anemia: A report of five cases. Am J
Med Sci 1965; 249:175-185.
December 2006
KUWAIT MEDICAL JOURNAL
Case Report
Carbamezepine Induced Pseudolymphoma
Shahid Aziz, Abdulkarim Al Aska, Ayman M Al Kharabah
Department of Medicine, King Saud University, Riyadh, Kingdom of Saudi Arabia
Kuwait Medical Journal 2006, 38 (4): 329-331
ABSTRACT
Aromatic anticonvulsants like phenytoin, carbamezepine,
and phenobarbitone are rarely associated with a
syndrome that mimics malignant lymphoma and is
known as pseudolymphoma syndrome (PLS). A 20-yearold female after being started on carbamezepine for
epilepsy for four weeks presented with two-week history
of high grade fever with chills and rigors, a generalized
itchy erythematous rash, lymphadenopathy, jaundice
and hepato-splenomegaly. Her complete blood count
(CBC) showed eosinophilia (17%) and liver function tests
(LFTs) showed marked elevation of transaminases and
direct hyperbilirubinemia. Lymph node biopsy showed
reactive hyperplasia. She improved dramatically after
stopping her carbamezepine therapy and is doing fine on
topiramate 400 mg orally twice daily. With a two year
follow up, there was no recurrence of the reported
symptoms. The differentiation of PLS from true
lymphoma is very important as making a wrong
diagnosis of malignant lymphoma in a patient with PLS
can be catastrophic.
KEYWORDS: anticonvulsant therapy, lymphoma
INTRODUCTION
Pseudo lymphoma syndrome is a rare side effect
of anticonvulsant therapy characterized by fever,
skin rash and lymphadenopathy that mimics
malignant lymphoma and mycosis fungoides. The
condition is potentially life threatening and
clinician awareness of this rare side effect of
anticonvulsant therapy is important because early
recognition and withdrawal of the offending agent
most of the times results in dramatic and complete
recovery, although death can occur with extensive
skin involvement, liver failure or agranulocytosis.
CASE REPORT
A 20-year-old female patient presented with a
two-week history of high grade fever with
sweating, chills and rigors. Fever was associated
with a generalized erythematous itchy rash all over
her body. For the last one week she also noticed
yellow discoloration of her eyes and skin with dark
colored urine. She had been on carbamezepine
therapy for tonic-clonic seizures for the past four
weeks. There was history of joint pains in all the
joints without redness or swelling and limitation of
movement on examination. She had a temperature
of 39 ºC, a pulse rate of 110/min and was jaundiced,
with bilateral submandibular, cervical and axillary
lymph nodes 2-3 cm in size, firm, non-tender and
mobile. There was an erythematous, maculopapular
rash involving her face, trunk, back and limbs with
scratch marks over it. She had hepato-splenomegaly
as well. Rest of her systemic examination was
u n remarkable. Her CBC and LFT results are
summarized in Table 1 and 2 respectively. Her chest
X-ray was normal. Serum carbamezepine level was
3.1 mg/ml and a throat swab showed no growth.
Her IgM antibodies to cytomegalovirus (CMV),
Epstein bar virus (EBV) and hepatitis A virus
(HAV) were negative, hepatitis B surface antigen
(HbsAg) and hepatitis C virus antibodies (HCVAb)
were also negative. Monospot test and antinuclear
antibodies (ANA) were negative. A b d o m i n a l
ultrasound confirmed hepato-splenomegaly and
no other intra-abdominal masses were detectable.
Echocardiography was normal. Her lymph node
biopsy showed reactive hyperplasia with no
malignant cells. Bone marrow aspiration and
biopsy was normal. Her carbamezepine was
stopped and she was started on topiramate for her
epilepsy. No systemic steroids were given. After
two days, her fever subsided and by the 5th day the
rashes started to fade out along with reduction in
the size of lymph nodes. She was discharged home
10 days after admission in good health and was
seen three months later in our outpatient clinic.
There were no palpable lymph nodes, liver or
spleen, her haematological indices and LFTs were
also found to be normal. With a two-year follow up,
there was no recurrence of the reported symptoms.
Address Correspondence to:
Dr. Shahid Aziz MRCP (UK), Department of Medicine (38), King Khalid University Hospital, P. O. Box 7805, Riyadh 11472, Kingdom of Saudi
Arabia. Fax; 0096614670999, E-mail: [email protected]
330
Carbamezepine Induced Pseudolymphoma
Table 1: Complete blood count
Table 2: Serum biochemistry and LFTs
On admission After 10 days After 3 months
WBC (X109/l)
HB (gm/dl)
MCV (fl)
MCH (pg)
Platelets (X109/l)
N
L
EOS
MONO
ESR (mm/hr)
5.30
11
84.3
28.4
286
41%
36%
17%
5%
15
December 2006
5.40
11.1
85
29.3
425
40%
44%
5%
11%
20
4.80
12
82.4
30
350
50%
39%
4%
6%
19
N: Neutrophils, L: Lymphocytes, EOS: Eosinophils, M: Monocytes
DISCUSSION
Carbamezepine is an aromatic anticonvulsant
with tricyclic structure related to phenytoin,
phenobarbital and primidone[1]. Pseudolymphoma
syndrome (PLS) is a rare side effect of carbamezepine
therapy but is well known with phenytoin therapy
as dilantin hypersensitivity syndrome[2] or phenytoin
syndrome[3]. Patricia Tennis et al [4], reported the risk
of developing hypersensitivity syndrome with
carbamezepine as 1 - 4.1 per 10,000 new users and
2.3 to 4.5 per 10,000 new users of phenytoin.
Some authorities suggested that we differentiate
between anticonvulsant hypersensitivity syndrome
and PLS on clinical ground but the differentiation
seems to be arbitrary as there is considerable
overlap in clinical presentation and histopathological
findings for the two entities[1,3]. Patients may present
with fever (75-100%) which is usually high grade
and swinging, skin rash (90%), facial edema (2588%), lymphadenopathy (63-70%) which may be
tender, hepatomegaly and hepatitis (25-60%),
myalgia and arthralgia (21%), pharyngitis (10%)[2,3].
Haematological abnormalities are protean and
range from lecuocytosis and leucopenia, agranulocytosis,
lymphocytosis, atypical lymphocytes, blast cells,
eosinophilia, monocytosis, pancytopenia, coagulation
disorders to hypo and hypergamma-globulinemia.
Our patient also showed eosinophilia of 17% in her
initial CBC, which returned to normal within two
weeks after withdrawal of the offending drug.
Hepatic injury is usually mild and most of the
times patients recover within a few weeks after the
cessation of causative agent. Failure to stop the
causative drug early may lead to more severe
hepatic injury[2,3] and severe hepatitis is a poor
prognostic sign. Death can occur due to liver
failure. Our patient showed marked impairment of
her liver function tests in the initial report in the
form of predominantly direct hyperbilirubinemia,
high alkaline phosphatase and transaminases,
which started to improve after the cessation of the
offending drug and returned to normal within
three months.
On admission
Urea (mmol/l)
Creatinine (µmol/l)
Total bilirubin(µmol/l)
Direct bilirubin(µmol/l)
Total proteins (gm/l)
Albumin (gm/l)
Alk Phos (U/l)
ALT (U/l)
AST (U/l)
GGT (U/l)
2.5
41
150
125
56
25
980
262
194
539
After 10 days
3.6
46
54
39
65
29
756
129
99
453
After 3 months
3.5
43
16
3
71
32
150
47
29
47
Alk Phos: Alkaline Phosphatase, ALT: Alanine amino transferase, AST:
Aspartate aminotransferase, GGT: Gamma glutamyl transferase
Lung involvement may occur in the form of
pneumonitis[1], bronchiolitis obliterans organizing
pneumonia (BOOP)[5], bronchial mucosal ulceration
and desquamation[6] which can be fatal. Serious
disturbances in pulmonary diffusion capacity may
be present even in the absence of changes on chest
X-ray[7].
Lymph node biopsy most of the times shows
reactive hyperplasia (as in our patient) but features
resembling malignant lymphoma may be seen such
as destruction of nodal architecture[8], atypical
lymphocytes with CD3, CD20, CD30 positivity[3,9,10]
and large cells indistinguishable from Reed
Sternberg cells[11]. Cutaneous biopsies may show
features resembling mycosis fungoides (MF) such
as epidermotrophism of atypical lymphocytes and
Partier’s microabscesses. However, features
favouring PLS over MF are the presence of marked
spongiosis, necrotic keratinocytes and eosinophilic
infiltrate in the epidermis, and in the dermis
papillary dermal edema, extravasated erythrocytes,
lymphocytes within the dermis larger than those in
epidermis and infiltration of various inflammatory
cells including neutrophils[3]. T cell receptor-γ gene
rearrangement studies may show monoclonal
rearrangement in PLS caused by valproate but not
in PLS caused by carbamezepine[3,9].
The exact pathophysiology of PLS is not known.
However, toxic metabolic theory proposed by Shear
and Spielberg[12] and Spielberg et al [13,14] seems to be
most appropriate. According to this theory aromatic
anticonvulsants (carbamezepine, phenytoin and
phenobarbital) are metabolized by cytochr ome
P450 to a toxic metabolite arene oxide, which is
detoxified by the enzyme epoxide hydrolase.
Deficiency of this enzyme leads to accumulation of
arene oxide in the body that acts as haptens[2,3,4]. This
also explains the cross reactivity seen between
aromatic anticonvulsants. Also the first degree
relatives of the patients with PLS are at increased
risk of developing the syndrome if exposed to
aromatic anticonvulsant due to the deficiency of the
December 2006
KUWAIT MEDICAL JOURNAL
enzyme epoxide hydrolase. An autosomal pattern
of inheritance has been suggested for this
deficiency[2]. But as PLS can be caused by valproate,
which has a different structure and is not
metabolized to arene oxide, it seems that other
mechanisms may operate, of which T-cell dysregulation
or dysfunction is one possibility.
Immediate management other than supportive
measures includes cessation of the causative agent
and this usually results in rapid recovery. Systemic
corticosteroids are of no benefit, but patients with
progressive disease despite cessation of causative
agent may benefit from them. However, data
supporting this, is lacking. For future control of
epilepsy in these patient anticonvulsants with a
different structure such as Lamotrigine, gabapentin
and topiramate can be used.
CONCLUSIONS
PLS is a rare side effect of carbamezepine
therapy for which early recognition and cessation
of the causative agent is important as it results in
dramatic and complete recovery. Death can occur in
PLS due to extensive skin involvement, liver failure
and agranulocytosis.
Once PLS occurs during the course of any
anticonvulsant therapy, this will affect the future
management of the underlying disorder for which
the anticonvulsant was used, as there is cross
reactivity between aromatic anticonvulsants and
valproate. Lamotrigine, gabapentin and topiramate
can be used in these patients. Aromatic anticonvulsants should be used with caution in first degree
relatives of the patients with PLS as they are at
higher risk of developing the syndrome.
REFERENCES
1.
David LNathan, Donald V Belsito. Carbamezepine induced
pseudo lymphoma with CD-30 Positive cells. J Am Acad
Dermatol 1998; 38:806-809.
2.
3.
4.
5.
6.
7.
8.
9.
10.
11.
12.
13.
14.
331
Carmela C Vittorio, Jennie J Muglia. Anticonvulsant
hypersensitivity syndrome. Arch Intern Med 1995;
155:2285-2290.
T S Choi, K S Doh, S H Kim, M S Jang, K S Suh, S T Kim.
Clinicopathological and genotypic aspects of anticonvulsantinduced pseudo lymphoma syndrome. Br J Dermatol 2003;
148:730-736.
Patricia Tennis, Robert S Stern. Risk of serious cutaneous
disorders after initiation of use of phenytoin, carbamezepine,
or sodium valproate. Neurology 1997; 49:542-46.
R Banka, M J Ward. Bronchiolitis obliterans and organizing
pneumonia caused by carbamezepine and mimicking
community acquired pneumonia. Postgrad Med J 2002;
78:621-622.
S E Handfield-Jones, R E Jenkins, S J Whittaker, C P Besse
and D HcGibbon. The anticonvulsant hypersensitivity
syndrome. Br J Dermatol 1993; 129:175-177.
Tijhvis GJ, Strijbos JH, Van Ermen A, Offerman JJ, Dubois
AE. Generalized side effects with the use of carbamezepine.
Ned Tijdshr Geneeskd 1995; 139:2265-2268.
Rispal P Lassuer C, Labouyrie E, Doutre MS, et al. Pseudo
lymphoma induced by carbamezepine. Rev Med Intern
1995; 16:214-218.
O Cogrel, M Beylot-Barry, B Vergier, et al. Sodium valproate
induced cutaneous pseudo lymphoma followed by
recurrence with carbamezepine. Br J Dermatol 2001;
144:1235-1238.
Yeo W, Chow J, Wong N, Chan AT, Johnson PJ.
Carbamezepine induced lymphadenopathy mimicking Ki-l
(CD30+) T-cell lymphoma. Pathology 1997; 29:64-66.
P Yates, G Stockdill, M McIntyre. Hypersensitivity to
carbamezepine presenting as pseudo lymphoma. J Clin
Pathol 1986; 39:1224-1228.
Shear NH, Spielberg SP. Anticonvulasnt hypersensitivity
syndrome: in vitro assessment of risk. J Clin Invest 1988;
82:1826-1832.
Spielberg SP, Gordon GB, Blake DA, Mellits DE, Bross DS.
Anticonvulsant toxicity in vitro: possible role of arene
oxides. J Pharmacol Exp Ther 1981;
217:386-389.
Spielberg SP, Gordon GB, Blake DA, Goldstein DA, Herlong
HF. Predisposition to phenytoin hepatotoxicity assessed in
vitro. N Engl J Med 1981; 305: 722-727.
332
KUWAIT MEDICAL JOURNAL
December 2006
Case Report
Walker-Warburg Syndrome: A Case Report
Magdy H Shafik1, Mohamed Taha Mohamed1, Talaat M Yousef2
Department of Pediatrics, Farwaniya Hospital, Kuwait
Department of Radiology, Farwaniya hospital, Kuwait
1
2
Kuwait Medical Journal 2006, 38 (4): 332-335
ABSTRACT
Congenital muscle dystrophy (CMD) is a group of
disorders characterized by significant muscle weakness
early in life. Two broad groups of CMD are recognized;
those with major brain anomalies and those without.
Walker-Warburg syndrome (WWS) belongs to the first
group. It is a rare autosomal recessive, genetically
heterogeneous disorder characterize by a triad of CMD,
brain and eye anomalies. Clinical features and brain
magnetic resonance imaging (MRI) findings previously
used to diagnose the syndrome remain valid.
In the presence of an affected sibling, prenatal diagnosis
is possible by fetal brain MRI and/or vaginal
sonography. Mapping of the WWS gene is still not
possible.
We report a Kuwaiti girl with WWS. The diagnosis was
based on clinical, neurophysiological and MRI findings.
To the best of our knowledge, this is the first case of WWS
to be reported, with some details, in the Arab population.
KEYWORDS: cobblestone cortex, congenital muscle dystrophy, type II lissencephaly
INTRODUCTION
The muscular dysfunction in children with
congenital muscle dystrophy (CMD) results from
deficiency or dysplasia of a group of proteins that
are vital for skeletal muscle action. Many of these
proteins play an important role during brain
development. That is why brain anomalies occur in
some groups of congenital muscle dystrophy.
Merosin (laminin α 2) is an example of the
skeletal muscle proteins. This, with other proteins,
is likely to have a regulatory role in neuronal
migration and organization of the cortex during
brain development.
Deficiency or dysfunction of some of these
proteins may explain the neuronal migration
defects (overmigration) in the group of CMD that is
associated with brain malformation [1].
Walker-Warburg Syndrome (WWS) is the most
severe form of CMD that is associated with brain
and eye anomalies. The diagnostic criteria for WWS
have been established by Dobyns et al[2] in 1989.
They suggested CMD, type II lissencephaly,
cerebellar malformation and ocular anomalies
(mainly retinal and anterior chamber malformation)
to be the principal diagnostic features of WWS.
Other brain anomalies, such as occipital
encephalocele, absent corpus callosum and fusion
of the hemispheres were reported in some patients
with WWS. Though not constant in all patients,
these anomalies were considered in favor of the
diagnosis of this syndrome and, in association with
the severity of the brain malformation, are helpful
in distinguishing WWS from another clinically
similar disorder, that is muscle - eye - brain disease
(MEB)[3].
CASE HISTORY
The patient was a fifteen- month-old girl, who
was born at term by an elective cesarean section.
She was the second child to a first cousin parents
with one healthy male sibling.
Aroutine antenatal ultrasonographic examination
at 24 weeks of gestation revealed cerebral ventriculomegaly. At birth, her weight (2.2 kg) and height
(44 cm) were just below the 5th percentile for age,
while the head circumference (36cm) was on the
95th percentile.
Examination revealed some dysmorphic features
in the form of brachycephalic skull, depressed
nasal bridge, widely spaced eyes with bilateral
corneal opacities, epicanthic folds and rocker
bottom feet deformity.
System review revealed a hypotonic baby with
absent deep tendons reflexes, poor muscle power
and weak sucking reflex. No other abnormal
findings could be detected.
Bilateral glaucoma with irido-corneal adhesions
(Peter’s anomaly) was diagnosed upon ophthalmological
evaluation.
Address correspondence to:
Dr. Magdy H. Shafik, Department of Pediatrics, Farwaniya hospital, P.O.box 43375, Hawally 32048, Kuwait. Tel: 00965-2626769, Mob: 009659535979, E- mail: [email protected]
December 2006
KUWAIT MEDICAL JOURNAL
333
Ü
ð
Fig. 2a
Fig. 1: Sagittal SE 440/22 image shows agyria, ventriculomegaly, thin
corpus callosum, collicular fusion, pontine and cerebeller hypoplasia, and
a distinctive dorsal kinking at the mesencephalic-pontine junction (a
forme fruste occipital encephalocele).
ð
Ü
î
Mesencephalic - pontine kinking
Thin corpus callosum
Collicular fusion
Routine biochemical investigations, screening
for congenital infections, inborn error of metabolism
and chromosomal anomalies were normal.
Cerebral computerized tomography (CT) at age
of one week confirmed the antenatal ultrasonographic findings of ventriculomegaly.
Serum creatinine phosphokinase (CK) enzyme
level was high (1400 U/l) at age of 10 days.
Nasogastric tube feeding was commenced in the
second week of life due to poor sucking and
frequent choking episodes. This is continued till
date.
Brain MRI at age of three weeks showed gross
ventriculomegaly, thin corpus callosum, pontine
and cerebellar hypolplasia, collicular fusion, dorsal
kinking of the brain stem, nearly complete agyria
and irregular gray-white matter junction, a pattern
characteristic of cobblestone lissencephaly.
A ventriculo-peritoneal shunt was inserted at
age of one month due to progressive head enlargement.
A repeated serum CK enzyme level at five and
twelve months of age revealed high levels (540 and
490 U/l respectively).
Electromyography (EMG) at age of 13 months
showed a myopathic pattern
Follow up examination of the child at age of 15
months showed that she is markedly hypotonic
with absent deep tendons reflexes and severely
failing to thrive {Weight (5kg), Height (63 cm) and
head circumference (40 cm) were all far below the
5th percentile for age}. Developmentally, she was
globally delayed with very poor visual and hearing
abilities.
Fig. 2b
Fig. 2 a & b: Axial (a) and coronal (b) SE 440/22 images shows vermian
hypoplasia, marked ventriculomegaly and smooth brain with
periventricular irregular low signal intensities representing irregular
cortical projections into the underlying white matter giving an irregular
gray - white matter junction
➮
irregular gray - white matter junction
DISCUSSION
WWS is a rare form of congenital muscle
dystrophy (CMD) which is associated with brain
malformation and eye anomalies. The first case was
reported by Walker [4] in 1942 who described a case
of lissencephaly (Greek, smooth brain) and eye
anomalies.
Familial occurrence was first reported by
Chemke et al[5] as he noted three out of seven siblings
of 3rd cousin parents were affected.
Warburg[6] reported several patients with hydrocephalus and retinal detachment. She suggested an
autosomal recessive inheritance noting the occurrence
of the syndrome in a sibling of related parents[7].
Myopathy was first reported by Williams et al [8] as
part of the syndrome.
In the past WWS was known as HARD ± E
syndrome (Hydrocephalus, Agyria, Retinal Dysplasia
± Encephalocele). The condition is usually lethal
334
Walker-Warburg Syndrome: A Case Report
within the first few months of life. Survival beyond
three years is unusual [3].
WWS shows some similarities with two other
syndromes, namely Muscle-Eye-Brain disease
(MEB) and Fukuyama muscle dystrophy (FMD). In
all these three syndromes there are muscle
dystrophies, eye anomalies and brain malformation.
WWS is the most severe form of the three
syndromes in terms of brain malformation[9].
Brain anomalies in WWS were given the term
“cobblestone complex” by Cormand et al[3]. These
anomalies include the neuropathological findings
of “cobblestone cortex” with multiple coarse gyri
and agyric regions[10].
Radiologicaly, MRI brain shows markedly
dilated lateral ventricles, irregular grey - white matter
junction, absent or hypoplastic corpus callosum,
flat brain stem and cerebellar hypoplasia with
minimal brain convolutions resembling lissencephaly[3].
These features are typically reported in the MRI
study of our patient (Fig. 1& Fig. 2 a & b).
The term “type II lissencephaly” (with
disorganized cortical layers) describes the minimal
brain convolutions in WWS, and is used to
characterize it from the classic 4 -layer ed
lissencephaly[2].
Occiptal encephalocele is in favour of the
diagnosis of WWS[3]. This is seen in our case as a
forme fruste (aborted form) with dorsal kinking of
the brain stem (Fig. 1).
Ocular anomalies in WWS include microphthalmia,
congenital cataract, retinal dysplasia, buphthalamus,
chamber dysgenesis, corneal clouding, Peter ’s
anomaly and congenital glaucoma (the last three
findings were reported in our case).
Congenital muscle dystrophy (CMD) as part of
the syndrome, has been shown in our case both
clinically (hypotonia with absent deep tendon reflex)
and by elevated CK on many occasions after the
age of six months, with myopathic pattern of EMG.
CK level normally can be as high as 700 U/l
immediately after delivery, but falls to normal
range (5-130U/l) by 6-10 weeks[11].
In patients with CMD, CK may reach thousands,
early in life, reflecting wide spread muscle necrosis
in the perinatal period. Later on, these patients
have low or normal CK because of lack of muscle
mass and limited mobility [9].
While the molecular genetic basis of FMD and
MEB disease are clearly identified, the molecular
and genetic basis of WWS is still unclear [3].
Mutation in O-mannosyltransferase gene (POMT1)
was found in 20% of patients with WWS phenotype
studied by Beltran et al[12]. They explained the severe
neuronal migration defect in WWS by mutation in
this gene. This gene encodes synthesis of an
December 2006
enzyme that catalyze the first step in synthesis of a
specific glycosylated protein called α-dystroglycan,
which is found in brain, muscles and peripheral
nerves of mammals [13].
However, POMT1 gene mutation was not found
in cases studied by Jiemenz et al[14] though they
found almost complete absence of α-dystroglycan
with mild reduction in laminin-alpha 2 (merosin) in
muscles of patients with WWS. They assumed that
muscle degeneration in WWS is due to defective αdystroglycan / laminin α 2 axis in the muscle
fiber’s basal lamina.
Moreover, mutation in fukutin gene (responsible
for Fukuyama muscle dystrophy) has been reported
by others[15,16] in patients with phenotypic features of
WWS. Their results confirm that WWS is a
genetically heterogenous condition.
Although the phenotypic features of the three
syndromes (WWS, FCMD, and MEB) might
overlap, lack of consistent ocular abnormalities in
FCMD allowed a clear clinical demarcation of this
syndrome. Moreover, identification of the gene
responsible for FCMD on chromosome 9 (q31q33)[17] allows this syndrome to be defined at
molecular and genetic level.
The presence of severe neurological changes
both clinically and in the cerebral MRI studies, as
reported in our patient, plus evidence of CMD are
considered enough for WWS to be clearly differentiated from MEB[3]. Moreover, the MEB gene was
recently localized to chromosome 1(p32-p34)[18], and
this allows MEB and WWS to be classified as
distinct disorders on both clinical and genetic
grounds.
Although molecular genetic study was not possible
in our case, the diagnosis was confirmed by the
typical clinical picture and the MRI findings in
association with evidence of CMD. This is in
keeping with the diagnostic criteria of WWS in
other literature[3,19].
Lack of consistent chromosomal abnormalities
in WWS makes prenatal diagnosis a difficult task.
However, prenatal diagnosis can be suspected by
fetal brain MRI [20] and/or transvaginal fetal
neurosonography[21]. Both methods allow lissencephaly
to be detected prenatally. This in association with
ventriculomegaly allows easy identification of an
affected fetus especially with positive family
history of a similar case. Proper counseling can thus
be provided for parents, taking in consideration the
poor prognosis of such condition.
ACKNOWLEDGEMENT
We are thankful to Dr Essam A Ismail,
Consultant in Pediatrics, Farwaniya Hospital
whose bright ideas helped the diagnosis of such a
case and also for his revision of the manuscript.
December 2006
KUWAIT MEDICAL JOURNAL
REFERENCES
Villanova M, Malandrini A, Toti P, et al. Localization of
merosin in the normal human brain : implications for
congenital muscular dystrophy with merosin deficiency. J
Submicrosc Cytol Pathol 1996; 41:173-180.
2. Dobyns WB, Pagan RA, Armstrong D, et al. Diagnostic
criteria for Walker- Warburg syndrome. Am J Med Genet
1989; 32:195-210.
3. Cormand B, Pihko H, Bayes M, Valanne L, et al. Clinical and
genetic distinction between Walker-Warburg syndrome and
muscle-eye-brain disease. Neurology 2001; 56:1059-1069.
4. Walker AE. Lissencephally. Arch Neurol Psychiatry 1942;
48:13-29.
5. Chemke J, Czernabilsky B, Mundel G, Barishaky YR. A
familial syndrome of central nervous system and ocular
malformation. Clin Genet 1975; 7:1-7.
6. Warburg M. Heterogeneity of congenital retinal nonattachment, falciforum folds, and retinal dysplasia . A guide
to genetic counseling. Hum Hered 1976; 26:137-148.
7. Warburg M. Hydrocephaly, congenital retinal non- attachment,
congenital falciform fold. Am J Ophthal 1978; 85:88-94.
8.
Williams RS, Swisher CN, Jennings M, Ambler M, Caviness
VS Jr. Cerebro-ocular dysgenesis (Walker-Warburg
syndrome): neuropathologic and etiologic analysis.
Neurology 1984; 34:1531-1541.
9. Mathews KD. Muscular dystrophy overview: genetic and
diagnosis. Neurol Clin 2003; 21:795-816.
10. Haltia M, Levio I, Somer H, et al. Muscle- eye- brain disease:
a neuropathological study. Ann Neurol 1997; 41:173-180.
11. Gilboa N, Swanson JR. Serum creatinine kinase in normal
newborn. Arch Dis Child 1976; 51:283-285.
12. Beltran D, Currier S, Steinberecher A, et al. Mutation in the
O-mannosyltransferase gene POMTI give rise to the severe
1.
13.
14.
15.
16.
17.
18.
19.
20.
21.
335
neuronal migration disorder Walker- Warburg syndrome.
Am J Hum Genet 2002; 71:1033-1043.
Sasaki T, Yamada H, Malsumura K, Shimizu T, Kobata A,
Endo T. Detection of O-mannosylglycans in rabbit skeletal
muscle alpha-dystroglycan. Biochem Biophys Acta 1998;
1425:599-606.
Jiemenez MC, Torelli S, Brown SC, et al. Profound skeletal
muscle depletion of alpha dystroglycan in WWS. Eur J
Pediatr Neurol 2003; 7:129-137.
Beltran D, Van Bokhoven H, Van Beusekom E, Van den
Akker W, et al. A homozygous nonsense mutation in the
fukutin gene causes a Walker-Warburg syndrome
phenotype. J Med Genet 2003; 40:845-848.
Silan F, Yoshioka M, Kobayashi K, et al. A new mutation of
Fukutin gene in a non- Japanese patient. Ann Neurol 2003;
53:392-396.
Kobayashi K, Nakahori Y, Miyake M, Matsumura K, et al.
An ancient retrotransposal insertion causes Fukuyamatype congenital muscle dystrophy. Nature 1998; 394:388392.
Cormand B, Avela K, Pikko H, et al. Assignment of muscleeye-brain disease gene to 1 p32-p34 by linkage analysis and
homozygosity mapping. Am J Hum Genet 1999; 64:126-135.
Dobyns WB, Kirkpalru JP, Hittner HM, Roberts R, Kretzer
FL, et al. Syndrome with lissencephaly II: Walker-Warburg
and cerebro-oculo-musclar syndrome and a new syndrome
with type II lisencephaly . Am J Med Genet 1985; 22:157195.
Okamura K, Murotsuki J, Sakai T, Matsumoto K, Shirane R,
Yajima A. Prenatal diagnosis of lissencephaly by magnetic
resonance image. Fetal diag Ther 1993; 8:56-59.
Ana M, Abdon A, Patricia M. Walker-Warburg syndrome,
case report and review of the literature. J Ultrasound Med
2001; 20:419-426.
KUWAIT MEDICAL JOURNAL
December 2006
Selected Abstracts of Articles Published
Elsewhere by Authors in Kuwait
Kuwait Medical Journal 2006, 38 (4): 336-338
Subjective Quality of Life of Outpatients with Diabetes: Comparison
with Family Caregivers’ Impressions and Control Group
Awadalla AW, Ohaeri JU, Tawfiq AM, Al-Awadi SA
Department of Psychiatry, Faculty of Medicine, Kuwait University, P.O. Box 24923, Safat, Kuwait 13110.
E-mail: [email protected]
J Natl Med Assoc. 2006; 98:737-745
Background: There is a paucity of studies on comparison of quality of life (QOL) of type-1 and type2 diabetes patients, and the impact of family caregivers’ impressions on the QOL of patients.
Objectives: To assess the subjective QOL of Sudanese diabetics using the WHOQOL-Bref, compared
with a general population sample; examine caregiver-patient concordance; and assess the variables
that impact on QOL.
Method: The responses of 105 outpatients with type-1 diabetes and 136 with type-2 diabetes were
compared with their family caregivers’ impressions and 139 general population subjects.
Results: Patients were predominantly dissatisfied with their life circumstances. Type-1 diabetics had
significantly lowest QOL scores, while the control group had highest scores. Having additional
medical problems; having diminished sexual desire; and being young, unemployed and single were
associated with poor QOL, but illness duration was not. Type-2 diabetics had lesser concordance with
caregivers. The only predictor of patients’ QOL was the caregivers’ impression of patients’ QOL.
Conclusions: Caregivers’ impression of patients’ QOL impacted on outcome. Caregiver education is,
therefore, important. The factors associated with QOL indicate a group that needs focused attention.
The good QOL for type-2 and nonsignificance of illness duration encourage therapeutic optimism.
The Effect of Seventy-Two-Hour Continuous Infusion of Long-acting
Natriuretic Peptide on Acute Ischemic Renal Failure in the Rat
Alhumoud HM
Department of Medicine, Division of Nephrology, Faculty of Medicine, College of Medicine, Kuwait University, Safat,
Kuwait. E-mail: [email protected]
Ren Fail 2006; 28:577-581
Objectives: Atrial natriuretic peptide (ANP(1-28)) protects the kidneys against acute renal failure in
animals; however, its use in humans has been disappointing. Long-acting natriuretic peptide
(LANP(1-30)) has natriuretic and diuretic actions similar to ANP(1-28), but it has a longer half-life and
a different receptor site. Therefore, this study’s aim was to determine if LANP(1-30) has better renal
protection than ANP(1-28), which may make it useful in the treatment of acute renal failure.
Subjects/Methods: Three groups of male Sprague-Dawley rats were used, each with a body weight
between 250-300 gm. Group 1 (ischemia only, n = 6) had a right nephrectomy followed by 30 minutes
of left renal pedicle clamping. Group 2 (LANP Peptide treated, n = 7) had renal ischemia similar to
Group 1, followed by an intraperitoneal bolus of 10 microg of LANP(1-30) and the placement of miniosmotic pumps delivering LANP(1-30) at a rate of 1 microg/hr for 72 hours. Group 3 (controls, n = 6)
was used to measure the baseline creatinine level and had no renal ischemia or surgery.
Results: Seventy-two hours post-renal ischemia, the weight loss in the ischemia group was similar to
the peptide treated group (7.65 +/- 1.14% and 10.03 +/- 0.9% body weight loss, respectively, p =
0.126). The ischemia group had significantly higher creatinine levels compared to the controls (66.3
+/- 5.3 versus 30.1 +/- 0.9 micromol/L, p = 0.002). The peptide-treated group had higher creatinine
(174.1 +/- 77.8 versus 66.3 +/- 5.3 micromol/L, p = 0.035) and LANP(1-30) levels (673.14 +/- 69.64
versus 45.83 +/- 8.45 pg/mL, p = 0.001) than the ischemia group.
Conclusion: Prolonged use of LANP(1-30) has no renal protective effect.
December 2006
KUWAIT MEDICAL JOURNAL
337
High Prevalence and Level of Resistance to Metronidazole, but Lack
of Resistance to Other Antimicrobials in Helicobacter Pylori, Isolated
from A Multiracial Population in Kuwait
John Albert M, Al-Mekhaizeem K, Neil L, Dhar R, Dhar PM, Al-Ali M, Al-Abkal HM, Haridas S.
Department of Microbiology, Faculty of Medicine, Kuwait University, Kuwait
Aliment Pharmacol Ther 2006; 24:1359-1366
Background: The primary treatment regimen for Helicobacter pylori infection for Kuwaitis does not
contain metronidazole, but that for expatriates does. There is also increasing failure of antimicrobial
therapy.
Aim: To determine the susceptibility of H. pylori from upper gastrointestinal biopsies of Kuwaitis and
non-Kuwaitis to find out if differences existed in the susceptibilities of the isolates from the two
different populations.
Methods: The susceptibilities of 96 H. pylori isolates were tested against metronidazole, amoxicillin,
clarithromycin and tetracycline by the E test. The rdxA gene was analysed from selected
metronidazole-susceptible and metronidazole-resistant strains to find out polymorphism and the
basis of metronidazole resistance.
Results: Approximately, 70% of isolates from both populations were metronidazole resistant with
65% isolates showing high minimum inhibitory concentration values of >256 mug/mL. No resistance
to the other three antimicrobials was found. There were novel nonsense and missense mutations with
no deletion in the rdxAgene by insertion of mini-IS605.
Conclusions: The prevalence and level of metronidazole resistance in H. pylori in the two
populations was high with no difference, in spite of different treatment regimens. Metronidazole
resistance in this transitional country appeared to be independent of prior metronidazole use for
treatment of H. pylori infection.
Determinants of Plasma Homocysteine in Relation to Hematological
and Biochemical Variables in Patients with Acute Myocardial Infarction
Marouf R, Zubaid M, Mojiminiyi OA, Qurtom M, Abdella NA, Al Wazzan H, Al Humood S
Department of Pathology, Kuwait University, Faculty of Medicine, Kuwait.
E-mail:[email protected]
South Med J 2006; 99:811-816
Background: Elevated plasma total homocysteine (tHcy) is a risk factor for coronary artery disease
(CAD), but the mechanism is not known. This study evaluates the determinants and associations of
tHcy in patients presenting with acute myocardial infarction (AMI).
Methods: Plasma concentration of tHcy, protein C, protein S, and antithrombin were measured in 210
(177 males and 33 females) patients with first AMI and 167 (87 males and 80 females) controls. Serum
vitamin B12, folate, creatinine, lipid profile, fasting glucose, full blood count and red cell folate were
determined. Creatinine clearance was calculated using the modification of diet in renal disease
formula. Univariate and multivariate analyses were used to determine the associations of tHcy.
Results: Mean tHcy was higher in male than female patients. On logistic regression analysis, the most
important determinants oftHcy in the patients were age, creatinine, creatinine clearance, vitamin B12
and red cell folate. When study patients were compared with the controls, tHcy, fasting glucose and
serum creatinine were significantly higher, while creatinine clearance and HDL cholesterol were
significantly lower in the study patients. Logistic regression analysis showed significant association
of tHcy with AMI, odds ratio = 1.39, in the presence of other confounding factors.
Conclusion: Our results show that tHcy is a significant risk factor for CAD in our patient population.
The determinants in the patients are age, glomerular filtration rate and the status of vitamins B12 and
folate. The above determinants should be kept in mind when using tHcy as a risk factor for CAD.
338
December 2006
Prevalence and Associations of Low Plasma Erythropoietin in
Patients with Type 2 Diabetes Mellitus
Mojiminiyi OA, Abdella NA, Zaki MY, El Gebely SA, Mohamedi HM, Aldhahi WA.
Department of Pathology, Faculty of Medicine, Kuwait University, Safat, Kuwait.
E-mail: [email protected]
Diabet Med. 2006; 23: 839-844
Aims: Low plasma erythropoietin (EPO) is a key causal factor in the anaemia of diabetic patients. The
aim of this study was to investigate the prevalence of anaemia in relation to EPO in patients with Type
2 diabetes.
Methods: In a clinic-based cross-sectional study of 161 Type 2 diabetes patients, we measured EPO,
ferritin and full blood count. The patients were classified on the basis of the urine albumin:creatinine
excretion ratio as normo-, micro- or macroalbuminuric. Serum creatinine, cystatin C and glomerular
filtration rate (GFR) calculated from cystatin C were used as markers of renal function. All the patients
were assessed for symptoms and signs of diabetic complications, including diabetic peripheral
sensory neuropathy (PSN).
Results: Twenty-one (13.0%) patients were anaemic; 80 patients (49.7%) had low EPO (< 5 mU/ml),
of whom 28.8% had a GFR < 60 ml/min per 1.73 m2; 57.5% were normoalbuminuric, 33.7% were
microalbuminuric and 8.8% macroalbuminuric. Although EPO was significantly higher in anaemic
patients compared with non-anaemic patients, the EPO response was inappropriate for the degree of
anaemia. Of patients with PSN, 66.7% had low EPO but there was no significant difference in EPO
between patients with and without PSN. Log EPO correlated significantly with urine
microalbumin:creatinine ratio and logistic regression analysis showed that haemoglobin, age and
urine microalbumin: creatinine ratio were the main determinants of EPO.
Conclusion: The degree of microalbuminuria is the most significant determinant of plasma EPO,
which is often low or inappropriately normal in diabetic patients with and without anaemia.
Treatment of Calculi in Kidneys with Congenital Anomalies: An
Assessment of the Efficacy of Lithotripsy
Al-Tawheed AR, Al-Awadi KA, Kehinde EO, Abdul-Halim H, Hanafi AM, Ali Y
Department of Surgery (Division of Urology), Mubarak Al-Kabeer Hospital, Safat, Kuwait.
Urol Res 2006; 34:291-298
We studied the effectiveness of extracorporeal shock wave lithotripsy (ESWL) in the treatment of
stones in kidneys with congenital anomalies to determine factors that may affect the results. Patients
found to have renal calculi in kidneys with different types of congenital anomalies were treated using
ESWL. All patients were investigated by intravenous urography (IVU) to confirm the diagnosis. J
stents were inserted prior to therapy in renal units with calculi exceeding 1.5 cm in diameter.
Complications encountered and factors affecting success using this treatment modality were
analysed. Twenty-five patients (18 males, 7 females) were studied between August 1988 and July
2005. There were nine patients with horseshoe kidneys, eight with ectopic kidneys, three with
malrotated kidneys, two with duplex renal system, and one patient each with polycystic kidneys and
hypoplastic kidney. The IVU showed 31 isolated calyceal or renal pelvic stones with mean stone
burden of 1.44cc. All 25 patients were treated by lithotripsy. Twenty-four (77.4%) renal units (in 19
patients) were completely cleared of stones, 2 (6.5%) renal units (2 patients) were partially cleared of
calculi and the procedures failed in 5 (16.1%) renal units (4 patients). Out of five renal units in which
the procedures failed, open surgery was performed in three renal units and percutaneous
nephrolithotomy (PCNL) was performed in two. None of the 25 patients developed any major
complications. No significant adverse changes in renal function tests were observed at 3-month
follow-up. The stone-free rate was influenced and reduced by stone size and location in the pelvicalyceal system. Calculi in kidneys with congenital anomalies may be treated successfully by ESWL
as a first-line therapy in the majority of patients. With position modifications, localization of stones
may be facilitated and disintegrated. The outcome in patients so treated does not differ significantly
from that in those with normal kidneys.
December 2006
KUWAIT MEDICAL JOURNAL
Forthcoming Conferences and Meetings
Compiled and edited by
Babichan K Chandy
Kuwait Medical Journal 2006, 38 (4): 339-342
Internal Medicine: Diabetes/Endocrinology
Dec 02-09, 2006
Tampa, FL, United States
Contact: Continuing Education Inc, 5700 4th St. N,
St. Petersburg FL 33703
Tel: 1-800-422-0711 / 727-526-1571; Fax: 727-527-3228
E-Mail: [email protected]
IDF 2006 19th World Diabetes Congress
Dec 05-07, 2006
Cape Town, South Africa
Contact: Congress Unit, International Diabetes
Federation, Avenue Emile De Mot 19, B-1000
Brussels
Tel: 32-25-431-631; Fax: 32-25-385-114
E-Mail: [email protected]
The Medical Management of AIDS: A
Comprehensive Review of HIV Management
Dec 07-09, 2006
San Francisco, CA, United States
Contact: UCSF Office of Continuing Medical
Education, 3333 California Street, Room 450, San
Francisco, CA94118
Tel: 415-476-4251 / 415-476-5808; Fax: 415-476-0318
/ 415-502-1795
E-Mail: [email protected]
Immunological Intervention in Human Disease
(A2)
Jan 06-11, 2007
Big Sky, MT, United States
Contact: Kellie McConnell
Tel: 800-253-0685 / 970-262-1230 ; Fax: 970-2621525
E-Mail: [email protected]
Obesity: Peripheral and Central Pathways
Regulating Energy Homeostasis (J2)
Jan 14 -17, 2007
Keystone, CO, United States
Contact: Kellie McConnell
Tel: 800-253-0685 / 970-262-1230; Fax: 970-262-1525
E-Mail: [email protected]
Mast Cells, Basophils, and IgE: Host Defense and
Disease (A6)
Jan 20 - 24, 2007
Copper Mountain, CO, United States
Contact: Kellie McConnell
Tel: 800-253-0685 / 970-262-1230 ; Fax: 970-2621525
E-Mail: [email protected]
Exacerbations of Airway Disease
Dec 08-10, 2006
San Juan, Puerto Rico
Contact: Roni LaVine
Tel: 732-438-0622; Fax: 732-438-6672
E-Mail: [email protected]
Modern Achievements of Cardiology in
Development of New Cardiological Products by
Results of Last Clinical Trials
Jan 30-31, 2007
Kiev, Ukraine
Contact: Dr Markov
Tel:38-0-632-776-465; Fax:38-0-445-331-270
E-Mail:[email protected]
Clinical Genetics
Dec 14-15, 2006
Coventry, England, United Kingdom
Contact: Dr Charlotte Moonan
Tel: 02-476-523-540; Fax: 02-476-523-701
E-Mail: [email protected]
Regional Asthma Congress
Jan 31 - Feb 02, 2007
Hurgada, Egypt
Contact: Prof.Kamal Maurice Hanna
Tel:20-105-310-087; Fax:20-24-186-586
E-Mail:[email protected]
Medical Devices, Ultrasound - 2006
Dec 16-17, 2006
Kiev, Ukraine
Contact: Dr Markov
Tel: 00-380-445-331-270 ; Fax: 00-380-445-331-270
E-Mail: [email protected]
Women’s Malignancies
Feb 02-04, 2007
Tehran, Iran
Contact: Dr Akbari or mrs Shadi
Tel: 00-982-122-724-090; Fax: 00-982-122-724-090
E-Mail: [email protected]
340
Forthcoming Conferences and Meetings
New Horizons in Anesthesiology
Feb 04-09, 2007
Steamboat Springs, CO, United States
Contact: Office of Continuing Medical Education
Tel:404-727-5695; Fax:404-727-5667
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Practical Updates in Anesthesiology
Feb 05-09, 2007
Puerto Vallarta, Puerto Rico
Contact: Jenny J. Mace
Tel:734-936-4235; Fax:734-936-9091
E-Mail:[email protected]
Clinical Audit 2007
Feb 06-07, 2007
London, England, United Kingdom
Contact: Clare Gallagher
Tel:02-0-85-411-399
E-Mail:[email protected]
45th Clinical Conference in Pediatric Anesthesiology
Feb 09-11, 2007
Anaheim, CA, United States
Contact: Tivi Ortiz
Tel:323-669-2262; Fax:323-660-8983
E-Mail:[email protected]
17th Symposium Intensive Medicine and Intensive Care
Feb 14-16, 2007
Bremen, Germany
Contact: Mrs. Kordula Grimm
Tel:00-49-0-421-3505-206; Fax:00-49-0-421-3505-340
E-Mail:[email protected]
Advances in Clinical Anesthetic Practice
Feb 17-21, 2007
Rancho Mirage, CA, United States
Contact: Shirley Jones
Tel:909-558-8173; Fax:909-558-0360
E-Mail:[email protected]
2nd Scientific Conference of the Saudi Cancer
Foundation: CANCER FORUM 2007
Feb 21-22, 2007
Al-Khobar, Saudi Arabia
Contact: Dr/ Ibrahim F. Al-Sheneber
Tel: 96-68-647-557; Fax: 96-638-649-884
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Mayo Clinic Symposium on Anesthesia and
Perioperative Medicine
Feb 21-24, 2007
Scottsdale, AZ, United States
Contact: Mayo Clinic Continuing Medical Education
Tel:480-301-4580; Fax:480-301-8323
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December 2006
10th Annual Conference of Indian Association of
Cardiovascular and Thoracic Anaesthesiologists
Feb 23-25, 2007
Chandigarh, India
Contact: Prof. GD Puri
Tel:91-1-722-756-509
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Difficult Airway Course: Anesthesia
Feb 23-25, 2007
Miami, FL, United States
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Tel:503-635-4761; Fax:404-795-0711
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Breast Cancer Managment and
Psychosocioeconomical Effect
Feb 23-25, 2007
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Contact: Dr Akbari or Mrs Shadi
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Tel:306-966-7787 / 306-766-4016; Fax:306-966-7673
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Imaging Immune Responses (J7)
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Third Oman International Anaesthesia and
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Feb 27, 2007 - Mar 01, 2007
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6th World Congress of the International Society
for Apheresis
Mar 02-04, 2007
Yokohama, Japan
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Tel: 440-358-1102; Fax: 440-358-1104
E-Mail: [email protected]
December 2006
KUWAIT MEDICAL JOURNAL
“IX International Symposium on Respiratory
Viral Infections”
Mar 03-07, 2007
Causeway Bay, Hong Kong
Contact: Roni LaVine
Tel:1-212-988-7732; Fax:1-212-717-1222
E-Mail:[email protected]
Immunologic Memory (C4)
Mar 03 - 08, 2007
Santa Fe, NM, United States
Contact: Kellie McConnell
Tel: 800-253-0685 / 970-262-1230; Fax: 970-262-1525
E-Mail: [email protected]
Advances in Internal Medicine
Mar 04-09, 2007
Park City, UT, United States
Contact: Jessica Kuo
Tel: 801-581-7606; Fax: 801-581-5393
E-Mail: [email protected]
The 2nd World Congress on Gender-Specific Medicine
Mar 08-11, 2007
Rome, Italy
Contact: Ms. Michal Pink
Tel: 9723-56-66-166; Fax: 972-3-56-66-177
E-Mail: [email protected]
Pediatric Anesthesiology 2007
Mar 08-11, 2007
Phoenix, AZ, United States
Contact: Society for Pediatric Anesthesia
Tel:804-282-9780; Fax:804-282-0090
E-Mail:[email protected]
Perioperative Management
Mar 11-14, 2007
Marco Island, FL, United States
Contact: Office of Continuing Medical Education
Tel:410-955-2959; Fax:410-955-0807
E-Mail:[email protected]
The 5th International Conference on Pain Control
and Regional Anaesthesia
Mar 14-18, 2007
Hong Kong, China
Contact: Jo Watling
Tel:00-448-700-132-930; Fax:00-448-900-132-940
E-Mail:[email protected]
CREF 27: The San Diego Cardiothoracic Surgery
Symposium: Science and Techniques of Perfusion
Mar 15-18, 2007
San Diego, CA, United States
Contact: Karen S. Morgan
Tel:1-805-534-0300; Fax:1-805-534-9030
E-Mail:[email protected]
341
9th Gastrointestinal Endoscopy Course & Workshop
Mar 18-20, 2007
Riyadh, Saudi Arabia
Contact: Department of Gastroenterology
Tel: 966-1-479-1000 Ext.5265 or 966-1-477-7714
Ext.6385; Fax: 966-1-476-0853
E-Mail: [email protected]
10th Mayo Clinic Endocrine Course
Mar 18-23, 2007
Kohala Coast, HI, United States
Contact: Dr. WF Young
Tel: 507-284-2509; Fax: 507-284-0532
E-Mail: [email protected]
Society of Cardiovascular Anesthesiologists 12th
Annual Update on Cardiopulmonary Bypass Mar
18-24, 2007
Whistler, BC, Canada
Tel:804-282-0084; Fax:804-282-0090
E-Mail:[email protected]
Difficult Airway Course: Anesthesia
Mar 19-22, 2007
Kahuku, HI, United States
Contact: Julie Vissers
Tel:503-645-4761; Fax:404-795-0711
E-Mail:[email protected]
STD Intensive
Mar 19-23, 2007
Cincinnati, OH, United States
Contact: Office of Continuing Education
Tel:1-800-207-9399 / 513-558-7277; Fax:513-5581708 / 513-558-1756
E-Mail:[email protected]
The 5th Annual Scientific Conference of The Saudi
Thoracic Society and The 24th Regional Meeting
of IUAT & LD
Mar 20-22, 2007
Riyadh, Saudi Arabia
Contact: Professor Mohamed Al-Hajjaj
Tel: 00-96-612-488-966; Fax: 00-96-612-487-431
E-Mail: [email protected]
Australasian Society for Infectious Diseases
Scientific Meeting 2007
Mar 22-24, 2007
Hobart, Australia
Contact: ASHM Conference Team
Tel:61-282-040-770; Fax:61-292-124-670
E-Mail:[email protected]
342
Forthcoming Conferences and Meetings
3rd World Congress Abdominal Compartment
Syndrome
Mar 22-24, 2007
Antwerp, Belgium
Contact: Werner Van Cleemputte, Managing
Director Medicongress Waalpoel 28/34, B-9960
Assenede, Belgium
Tel:32-0-93-443-959; Fax:32-0-93-444-010
E-Mail:[email protected]
Obstetrical Anesthesia 2007
Mar 22-25, 2007
San Francisco CA United States
Contact: Office of Continuing Medical Educaton
Tel:415-476-5808; Fax:415-502-1795
2nd International Congress of Molecular
Medicine
Mar 24-28, 2007
Istanbul, Turkey
Contact: Prof. Dr.Turgay Isbir
Tel: 90-2-126-351-959; Fax: 90-2-126-351-959
E-Mail: [email protected]
HIV Vaccines: From Basic Research to Clinical
Trials (X7)
Mar 25-30, 2007
Whistler, BC, Canada
Contact: Kellie McConnell
Tel: 800-253-0685 / 970-262-1230; Fax: 970-262-1525
E-Mail: [email protected]
Molecular and Cellular Determinants of HIV
Pathogenesis (X8)
Mar 25-30, 2007
Whistler, BC, Canada
Contact: Kellie McConnell
Tel: 800-253-0685 / 970-262-1230; Fax: 970-262-1525
E-Mail: [email protected]
December 2006
27th International Symposium on Intensive Care
and Emergency Medicine
Mar 27-30, 2007
Brussels, Belgium
Contact: Marcos Garcia
Tel:32-25-553-631; Fax:32-25-554-555
E-Mail:[email protected]
4th International Symposium on Diabetes and
Pregnancy
Mar 29-31, 2007
Istanbul, Turkey
Contact: Amy Altwerger
Tel: 41-229-080-488; Fax: 41-22-732-285
E-Mail: [email protected]
New Horizons in Anesthesiology
Apr 01-06, 2007
Cozumel, Mexico
Contact: Office of Continuing Medical Education
Tel:404-727-5695; Fax:404-727-5667
E-Mail:[email protected]
International Scientific Congress for Young
Doctors
Apr 04-08, 2007
Donetsk, Ukraine
Contact: Anatoliy
Tel:8-10-380-050-211-54-33; Fax:8-10-380-062-33455-39
E-Mail:[email protected]
The International Conference on Transfusion
Medicine
May 07-09, 2007
Tehran, Iran
Contact: Meeting Organiser
Tel:982-188-601-573; Fax:982-188-601-573
E-Mail:[email protected]
11th Pan Arab Conference on Diabetes PACD11
Mar 27-30, 2007
Cairo, Egypt
Contact: Mahmoud Ibrahim MD
Tel: 20-122-131-868 / 20-101-560-794; Fax: 20-22723-693 / 20-22-564-365
E-Mail: [email protected]
International Workshop on Tuberculosis Vaccines
2007 - TBVaccines2007
May 13-17, 2007
Varadero Beach, Matanzas, Cuba
Contact: Dr. Armando Acosta / Dr. Mar’a Elena
Sarmiento
Tel:537-216-911; Fax:537-208-6075
E-Mail:[email protected]
First International Conference on E-Medicine
Mar 27-30, 2007
Cairo, Egypt
Contact: Amr Ibrahim
Tel: 20-122-131-868 / 20-101-560-794; Fax: 2022723-693
E-Mail: [email protected]
10th Jubilee International Multidisciplinary
Neuroscience Conference Stress and Behavior
May 16-19, 2007
St. Petersburg, Russia
Contact: Dr. Allan V. Kalueff, Conference Chair
Tel: 358-0-442-865-613
E-Mail: [email protected]
December 2006
KUWAIT MEDICAL JOURNAL
Interventional Ultrasound - Clinical applications
May 21-23, 2007
City: Ravello - Amalfi Coast, Italy
Contact:Dr. L.Tarantino
Tel: 39-0-818-817-059; Fax: 39-0-818-891-302
E-Mail: [email protected]
Neurologic Emergencies and Neurocritical Care
May 22-25, 2007
City: New York ,NY Country, United States
Contact:Center for Continuing Education,
Columbia University, College of Physicians &
Surgeons, 630 West 168th Street, Unit 39, New
York, NY 10032
Tel: 212-305-3334; Fax: 212-781-6047
E-Mail: [email protected]
ICN Conference, CNR and Regulation Conference
May 27- Jun 03, 2007
City:Yokohama, Japan
Contact:Marije Wiegerinck
Tel : 31-205-040-203; Fax:31-205-040-225
E-Mail:[email protected]
11th Congress of the Movement Disorder Society
June 03-07, 2007
City:Istanbul, Turkey
Contact: The Movement Disorder Society, 611 East
Wells Street, Milwaukee, WI 53202 USA Tel: 1-414276-2145; Fax: 1-414-276-3349
E-Mail: [email protected]
HIV/AIDS 2007
Jun 06-11, 2007
Kololi, Gambia
Contact: Anthony F. England, Ph.D.
Tel: 31-302-145-715; Fax: 31-302-145-715
E-Mail: [email protected]
2nd International Congress on Neuropathic
Congress
June 07-10, 2007
City:Berlin, Germany
Contact :Ilana Eliav
Tel : 41-229-080-488; Fax: 41-227-322-850
E-Mail: [email protected]
3rd International Workshop on HIV and Hepatitis
Co-infection
June 07-09, 2007
City: Paris, France
Contact: Jo-Els van der Woude
Tel: 31-302-307-147; Fax:31-302-307-148
E-Mail: [email protected]
343
4th World Congress of the International Society of
Physical and Rehabilitation Medicine
June 10-14, 2007
City:Seou, Korea, Republic of
Contact: 4th ISPRM Secretariat
Tel: 82-2-566-6339 Fax:82-2-565-2434
E-Mail: [email protected]
3rd International Congress on Gastrointestinal
Oncology
June 14-16, 2007
City: Hersonissos, Crete island, Greece
Contact: Mrs Tina Fragkaki
Tel: 302-109-730-697; Fax: 302-109-767-208
E-Mail: [email protected]
Well Aging, Andropause, Menopause
June 15-16, 2007
City: Luxembourg, Luxembourg
Contact: Monardo Claudine
Tel: 35-226-264-134; Fax:35-226-264-175
E-Mail:[email protected]
3rd International Conference on Birth Diseases
and Disabilities
Jun 17-22, 2007
Rio de Janeiro, Brazil
Contact: Monica Cevidanes, PMP
Tel: 55-212-266-9150; Fax: 55-212-266-9175
E-Mail: [email protected]
Clinical Trials Results of Gastroenterological
Products, Practical Value from the Point of View of
Evidence Medicine
Jun 19-20, 2007
City: Kiev, Ukraine
Contact: Dr Markov
Tel: 38-0-632-776-465; Fax: 38-0-445-331-270
E-Mail: [email protected]
Diabetes Camp
June 23-30, 2007
City: Seattle, WA, United States
Contact: Sandra Barnhart
Tel: 1-800-422-0711; Fax:727-527-3228
E-Mail: [email protected]
17th International Epilepsy Symposium: Epilepsy
Surgery
June 27-29, 2007
City: Cleveland, OH, United States
Contact: The Cleveland Clinic Center for
Continuing Education, 9500 Euclid Ave. KK31,
Cleveland, Ohio 44195
Tel: 954-659-5490 / 800-762-8173 / 216-444-5696;
Fax:954-659-5491
E-Mail:[email protected]
KUWAIT MEDICAL JOURNAL
December 2006
WHO-Facts Sheet
1. New Global Estimates to Mark World Sight Day
2. A Clean Bill for Indoor Use of DDT to Control Malaria
3. Emergence of XDR-TB
4. Call for Intensified Action to Halt a Quarter of a Million TB/HIV Deaths a Year
5. Helmet Use Saves Lives
Compiled and edited by
Babichan K Chandy
Kuwait Medical Journal 2006, 38 (4): 344-348
1. NEW GLOBAL ESTIMATES TO MARK
WORLD SIGHT DAY
Sight test and glasses could dramatically improve
the lives of 150 million people with poor vision
A simple sight test and eyeglasses or contact
lenses could make a dramatic difference to the lives
of more than 150 million people who are suffering
from poor vision. Children fail at school, adults are
unable to work and families are pushed into
poverty as a result of uncorrected visual impairment.
To mark World Sight Day, 12 October 2006, the
World Health Organization (WHO) has released
new global estimates which, for the first time,
reveal that 153 million people around the world
have uncorrected refractive errors (more commonly
known as near-sightedness, far-sightedness and
astigmatism). Refractive errors can be easily
diagnosed, measured and corrected with eyeglasses
or contact lenses, yet millions of people in low and
middle income countries do not have access to
these basic services.
Without appropriate optical correction, millions
of children are losing educational opportunities
and adults are excluded from productive working
lives, with severe economic and social consequences.
Individuals and families are frequently pushed
into a cycle of deepening poverty because of their
inability to see well. At least 13 million children
(age 5 to 15) and 45 million working-age adults
(age 16 to 49) are affected globally. Fully 90% of all
people with uncorrected refractive errors live in
low and middle income countries.
“These results reveal the enormity of the
problem,” said Dr Catherine Le Galès-Camus,
WHO Assistant Director-General, Noncommunicable Diseases and Mental Health. “This
common form of visual impairment can no longer
be ignored as a target for urgent action.”
WHO previously estimated that 161 million
people were visually impaired from eye diseases
such as cataract, glaucoma and macular degeneration.
Uncorrected refractive errors were not included in
these earlier estimates. These latest WHO estimates
add to the previous number and effectively double
the estimated total number of visually-impaired
people worldwide, bringing it to some 314 million
people globally. The estimates also confirm that
uncorrected refractive errors are a leading cause of
visual impairment worldwide.
As part of the VISION 2020 Global Initiative to
eliminate avoidable visual impairment and
blindness worldwide, WHO has been working with
its partners to improve access to affordable eye
exams and eyeglasses for people in low and middle
income countries. This new information concerning
the prevalence of refractive errors will strengthen
the efforts of the VISION 2020 partnership to raise
awareness of the magnitude of the problem and
spur increased commitment for action.
“Correction of refractive errors is a simple and
cost-effective intervention in eye care,” said Dr
Serge Resnikoff, Coordinator of WHO’s Chronic
Disease Prevention and Management unit. “Now
that we know the extent of the problem of
uncorrected refractive errors, especially in low and
middle income countries, we must re-double our
efforts to ensure that every person who needs help
is able to receive it.”
Note: Refractive errors occur when the eye is not
able to correctly focus images on the retina. The
result is blurred vision, which is sometimes so
severe that it creates functional blindness for
affected individuals.
The three most common refractive errors are:
l Myopia (nearsightedness) - this is difficulty in
seeing distant objects clearly.
l Hyperopia also known as Hypermetropia
Address correspondence to: Office of the Spokesperson, WHO, Geneva. Tel.: (+41 22) 791 2599; Fax (+41 22) 791 4858; Email: [email protected]; Web
site: http://www.who.int/
December 2006
KUWAIT MEDICAL JOURNAL
(farsightedness) - this is difficulty is seeing close
objects clearly.
l Astigmatism - This is distorted vision
resulting from an irregularly curved cornea.
For more information contact:Alexandra Touchaud,
Communication officer, WHO Geneva, Tel: +41 22 791
5053, Mobile: +41 79 754 7763, Email:
[email protected]. Dr JoAnne Epping-Jordan, Senior
Programme Adviser, WHO Geneva, Tel. direct: +41 22
791 4646, Email: [email protected].
2. A CLEAN BILL FOR INDOOR USE OF
DDT TO CONTROL MALARIA
WHO promotes indoor spraying with insecticides
as one of three main interventions to fight
Malaria
Nearly thirty years after phasing out the
widespread use of indoor spraying with DDT and
other insecticides to control malaria, the World
Health Organization (WHO) today announced that
this intervention will once again play a major role
in its efforts to fight the disease. WHO is now
recommending the use of indoor residual spraying
(IRS) not only in epidemic areas but also in areas
with constant and high malaria transmission,
including throughout Africa.
“The scientific and programmatic evidence
clearly supports this reassessment,” said Dr Anarfi
Asamoa-Baah, WHO Assistant Director-General
for HIV/AIDS, TB and Malaria. “Indoor residual
spraying is useful to quickly reduce the number of
infections caused by malaria-carrying mosquitoes.
IRS has proven to be just as cost effective as other
malaria prevention measures, and DDT presents no
health risk when used properly.”
WHO actively promoted indoor residual
spraying for malaria control until the early 1980s
when increased health and environmental concerns
surrounding DDT caused the organization to stop
promoting its use and to focus instead on other
means of prevention. Extensive research and
testing has since demonstrated that well-managed
indoor residual spraying programmes using DDT
pose no harm to wildlife or to humans.
“We must take a position based on the science
and the data,” said Dr Arata Kochi, Director of
WHO’s Global Malaria Programme. “One of the
best tools we have against malaria is indoor
residual house spraying. Of the dozen insecticides
WHO has approved as safe for house spraying, the
most effective is DDT.”
Indoor residual spraying is the application of
long-acting insecticides on the walls and roofs of
houses and domestic animal shelters in order to kill
345
malaria-carrying mosquitoes that land on these
surfaces.
“Indoor spraying is like providing a huge
mosquito net over an entire household for aroundthe-clock protection,” said U.S. Senator Tom Coburn,
a leading advocate for global malaria control efforts.
“Finally, with WHO’s unambiguous leadership on the
issue, we can put to rest the junk science and myths
that have provided aid and comfort to the real
enemy - mosquitoes - which threaten the lives of
more than 300 million children each year.”
Views about the use of insecticides for indoor
protection from malaria have been changing in
recent years. Environmental Defense, which
launched the anti-DDT campaign in the 1960s, now
endorses the indoor use of DDT for malaria control,
as does the Sierra Club and the Endangered
Wildlife Trust. The recently-launched President’s
Malaria Initiative (PMI) announced last year that it
would also fund DDT spraying on the inside walls
of households to prevent the disease.
Programmatic evidence shows that correct and
timely use of indoor residual spraying can reduce
malaria transmission by up to 90 percent. In the
past, India was able to use DDT effectively in
indoor residual spraying to cut dramatically the
number of malaria cases and fatalities. South Africa
has again re-introduced DDT for indoor residual
spraying to keep malaria case and fatality numbers
at all-time low levels and move towards malaria
elimination. Today, 14 countries in Sub-Saharan
Africa are using IRS and 10 of those are using DDT.
The World Health Organization also called on
all malaria control programmes around the world
to develop and issue a clear statement outlining
their position on indoor spraying with long-lasting
insecticides such as DDT, specifying where and
how spraying will be implemented in accordance
with WHO guidelines, and how they will provide
all possible support to accelerate and manage this
intervention effectively.
“All development agencies and endemic
countries need to act in accordance with WHO’s
position on the use of DDT for indoor residual
spraying,” said Richard Tren, Director of Africa
Fighting Malaria. “Donors in particular need to
help WHO provide technical and programmatic
support to ensure these interventions are used
properly.”
Indoor residual spraying is one of the main
interventions WHO is now promoting to control
and eliminate malaria globally. A second is the
widespread use of insecticide-treated mosquito
nets. While the use of bed nets has long been
encouraged by WHO, the recent development of
“long-lasting insecticidal nets” (LLINs) has
346
WHO-Facts Sheet
dramatically improved their usefulness. Unlike
their predecessors, the long-lasting nets need not be
re-dipped in buckets of insecticide every six
months as they remain effective for up to five years
without retreatment.
Finally, for those who do ultimately become sick
with malaria, more effective medicines are
increasingly becoming available. Unlike previous
antimalarials that have been rendered useless in
many regions due to drug resistance, Artemisinin
Combination Therapies (ACTs) are now recommended. These lifesaving medications are becoming
more widely available throughout the world. In
January of this year, WHO took stringent measures
to help prevent future resistance to antimalarial
medicines by banning the use of malaria
monotherapy. An example of the negative
consequences of drug resistance is apparent in the
threat it poses to intermittent preventive treatment
in pregnancy (IPTp), a crucial strategic intervention
to protect pregnant women from the consequences
of malaria.
Each year, more than 500 million people suffer
from acute malaria, resulting in more than one
million deaths. At least 86 percent of these deaths
are in sub-Saharan Africa. Globally an estimated
3,000 children and infants die from malaria every
day and 10,000 pregnant women die from malaria
in Africa every year. Malaria disproportionately
affects poor people, with almost 60 percent of
malaria cases occurring among the poorest 20
percent of the world’s population.
For more information contact: In Washington, DC:
Jim Palmer at 1 (202) 262-9823, or Michael Riggs at 1
(202) 669-2163. In Geneva: Ed Vela at +41 22 7914550 or Shiva Murugasampillay at +41 22 791-1019.
3. EMERGENCE OF XDR-TB
WHO concern over extensive drug resistant TB
strains that are virtually untreatable
The World Health Organization (WHO) has
expressed concern over the emergence of virulent
drug-resistant strains of tuberculosis (TB) and is
calling for measures to be strengthened and
implemented to prevent the global spread of the
deadly TB strains. This follows research showing
the extent of XDR-TB, a newly identified TB threat
which leaves patients (including many people
living with HIV) virtually untreatable using
currently available anti-TB drugs.
What is XDR-TB?
MDR-TB (Multidrug Resistant TB) describes
strains of tuberculosis that are resistant to at least
the two main first-line TB drugs - isoniazid and
December 2006
rifampicin. XDR-TB, or Extensive Drug Resistant
TB (also referred to as Extreme Drug Resistance) is
MDR-TB that is also resistant to three or more of the
six classes of second-line drugs.
The description of XDR-TB was first used earlier
in 2006, following a joint survey by WHO and the
US Centers for Disease Control and Prevention
(CDC).
Resistance to anti-TB drugs in populations is a
phenomenon that occurs primarily due to poorly
managed TB care. Problems include incorrect drug
prescribing practices by providers, poor quality
drugs or erratic supply of drugs, and also patient
non-adherence.
What is the current evidence of XDR-TB?
Recent findings from a survey conducted by
WHO and CDC on data from 2000-2004 found that
XDR-TB has been identified in all regions of the
world but is most frequent in the countries of the
former Soviet Union and in Asia.
Scarce drug resistance data available from
Africa indicate that while population prevalence of
drug resistant TB appears to be low compared to
Eastern Europe and Asia, drug resistance in the
region is on the rise.
Given the underlying HIV epidemic, drugresistant TB could have a severe impact on
mortality in Africa and requires urgent
preventative action.
What action is required to prevent XDR-TB?
XDR-TB poses a grave public health threat,
especially in populations with high rates of HIV
and where there are few health care resources.
Recommendations outlined in the WHO
Guidelines for the Programmatic Management of
Drug Resistant Tuberculosis include:
l strengthen basic TB care to prevent the
emergence of drug-resistance
l ensure prompt diagnosis and treatment of
drug resistant cases to cure existing cases and
prevent further transmission
l increase collaboration between HIV and TB
control programmes to provide necessary prevention
and care to co-infected patients
l increase investment in laboratory infrastructures
to enable better detection and management of
resistant cases.
For more information contact: Glenn Thomas, Stop
TB Department, WHO, Mobile: +41 79 509 0677,
email: [email protected]. Dr Karin Weyer, Director,
South African Medical Research Council, Unit for TB
Operational and Policy Research, Tel: +27.12.339-8550,
Mobile: +27 82 4608836, email: [email protected].
December 2006
KUWAIT MEDICAL JOURNAL
4. CALL FOR INTENSIFIED ACTION TO
HALT A QUARTER OF A MILLION TB/HIV
DEATHS A YEAR
“Joint TB and HIV interventions can save lives
and must be accelerated” says international Aids
society president
Leading HIV experts called on the global HIV
community to intensify collaboration on tuberculosis
control, to prevent the deaths of a quarter of a
million people living with HIV (PLHIV) a year.
At the XVI International AIDS Conference in
Toronto this year, HIV Director Dr Kevin De Cock
and TB/HIV Coordinator Dr Paul Nunn, both from
WHO, were joined by Dr Helene Gayle, the
International AIDS Society President. Together,
they urged HIV health workers to target and scaleup joint activities for tuberculosis and HIV.
“TB prevention, diagnostic and treatment
services must become core functions of all HIV
services,” said Dr De Cock. “People living with
HIV are more vulnerable to TB, even if they’re on
antiretroviral therapy. TB can be treated and cured
so most of these deaths are absolutely preventable.
HIV policy-makers, health ministers and health
workers all have a vital role in making sure that
deaths from TB are reduced.”
“Joint TB and HIV interventions can save lives
and must be accelerated,” said Dr Gayle. “More
than a third of all people infected with HIV are also
infected with the tuberculosis bacillus, which
causes the deaths of a quarter of a million people
living with HIV, every year.”
“This is important research which shows that
TB preventive treatment is successful in reducing
TB cases in PLHIV, even for those who are already
taking life-saving antiretroviral drugs.” said Dr
Richard Chaisson, Principal Investigator a Brazilbased study. He also emphasized that research into
new TB drugs, diagnostics and vaccines appropriate
for PLHIV, and operational studies and effective
models to deliver the services to those who need
them, are urgently needed.
“We have the essential know-how and policy
guidance to address TB among PLHIV and
progress has been documented. However, the
progress has been slow, compared to the scale of
the problem,” said Dr Paul Nunn of WHO’s Stop
TB Department.
“In countries dually affected by TB and HIV
these interventions should be rapidly scaled up
and implemented through effective collaboration
between HIV and TB control programmes, and
general health services. Two years ago, Nelson
Mandela warned the world that ‘We can’t fight
AIDS unless we do much more to fight TB.’ “Mr
Mandela’s warning on HIV and TB still needs to be
347
translated into large scale action. Commitments
made at the G8, UN and African Union summits
must be experienced by the actual communities
most affected by the dual epidemics, particularly in
Africa where HIV-related TB deaths are the highest
in the world”.
Globally, TB is second only to HIV as an
infectious killer of adults, causing nearly nine
million cases of active TB disease and two million
deaths every year. In countries with a high
prevalence of TB, HIV programmes must scale up
TB prevention, diagnosis and treatment.
For more information contact: In Toronto: Carole
Francis, Tel: +41 79 54 079 56, email:
[email protected]. Glenn Thomas, Tel: +41 79 50 906
77, [email protected]
5. HELMET USE SAVES LIVES
Increasing helmet use promoted as an effective
method of reducing road injuries and deaths
Each year, about 1.2 million people die as a
result of road traffic crashes, and millions more are
injured or disabled. Most of the deaths are
preventable. In many low-income and middleincome countries, users of two-wheelers particularly motorcyclists - make up more than 50%
of those injured or killed on the roads. Head
injuries are the main cause of death and disability
among motorcycle users, and the costs of head
injuries are high because they frequently require
specialized medical care or long-term rehabilitation.
Wearing a helmet is the single most effective
way of reducing head injuries and fatalities
resulting from motorcycle and bicycle crashes.
Wearing a helmet has been shown to decrease the
risk and severity of injuries among motorcyclists by
about 70%, the likelihood of death by almost 40%,
and to substantially reduce the costs of health care
associated with such crashes.
The World Health Organization (WHO) is
intensifying efforts to support governments,
particularly those in low-income and middleincome countries, to increase helmet use through a
new publication, Helmets: a road safety manual for
decision-makers and practitioners.
The manual is a follow-up to the World report
on road traffic injury prevention, published in 2004
by WHO and the World Bank, which provided
evidence that establishing and enforcing
mandatory helmet use is an effective intervention
for reducing injuries and fatalities among twowheeler users. The manual has been produced
under the auspices of the UN road safety
collaboration, in collaboration with the Global
Road Safety Partnership, the FIA Foundation for
348
WHO-Facts Sheet
the Automobile and Society, and the World Bank, as
one of a series of documents that aim to provide
practical advice on implementing the recommendations of the World Report.
The importance of increasing helmet use follows
dramatic growth in motorization around the world,
largely from increasing use of motorized twowheelers, particularly in Asian countries. In China,
for example, motorcycle ownership over the last
ten years has increased rapidly. In 2004, it was
estimated that more than 67 million motorcycles
were registered in the country, and approximately
25% of all road traffic deaths were among
motorcyclists and their passengers.
“We want to make helmet use a high priority for
national public health systems,” says Dr. Anders
Nordström, Acting Director-General of WHO. “We
need to stress not only the effectiveness of helmets
in saving lives, but the fact that helmet programmes
are good value for money. Countries will recoup
their investment in these programmes many times
over through savings to their health care systems,
as well as savings to other sectors.”
Many countries have succeeded in raising rates
of helmet use through adopting laws that make
helmet use compulsory, enforcing these laws, and
raising public awareness about the laws, as well as
the benefits of helmet use. This new helmet manual
draws on such examples.
In Thailand, for instance, 80% of the 20 million
registered motorized vehicles are motorcycles. In
1992, when helmet use was not mandatory, 90% of
deaths resulting from traffic injuries were among
motorcycle users, almost all due to head injuries.
Legislation passed in the north-eastern province of
Khon Kaen to make helmet use mandatory,
supported by enforcement and publicity programmes,
led to a 40% reduction in head injuries among
motorcyclists and a 24% drop in motorcyclist
December 2006
deaths within the two years
This new manual provides technical advice to
governments on the steps needed to assess current
helmet use, and then design, implement and
evaluate a helmet use programme. The manual
addresses specific issues pertinent to many lowincome and middle-income countries, such as:
l What can be done to protect the large number
of children who ride as passengers on their parents’
motorcycles?
l Are there financial disincentives in place that
make helmets unaffordable and thus reduce their
use, for example, sales tax, or import duties that
could be removed by governments in efforts to
increase helmet use?
l How can enforcement be consistent and
effective when resources are constrained? Should
countries aim to implement a comprehensive
helmet law, or is it more appropriate to phase in a
law, in order to allow the traffic police to manage
the new responsibility?
The manual will be implemented in a number of
countries over the next two years, starting in the
ASEAN region through the Global Road Safety
Partnership’s GRSI initiative, but extending to
cover countries from Africa, Latin America and the
Middle East.
In addition to the publication of this manual,
WHO has also established a network of experts
working to increase helmet use, and supports
helmet programmes directly in its country work on
road safety.
For more information contact: Laura Sminkey,
Communications Officer, Department of Injuries and
Violence Prevention, WHO/Geneva, tel: +41 22 791
4547 e-mail: [email protected]
December 2006
THE
KUWAIT MEDICAL JOURNAL
Yearly Author Index
Kuwait Medical Journal
(KMJ) 2006; Volume 38
The Kuwait Medical Journal 2006, 38 (4): 353-354
Abdelhadi MSA . . . . . . . . . . . . . . . . . . . . . . . . . . 37
Abdelkader B . . . . . . . . . . . . . . . . . . . . . . . . . . . 276
Aboobacker KC . . . . . . . . . . . . . . . . . . . . . . . . . 147
Abu Tiban FMA . . . . . . . . . . . . . . . . . . . . . . . . . 144
Abubacker S . . . . . . . . . . . . . . . . . . . . . . . . . . . . 238
Akbar MAJ . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 226
Akhtar S . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 33
Akhtar SS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 132
Al Akkad M . . . . . . . . . . . . . . . . . . . . . . . . . . . . 300
Al Aska A . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 329
Al Duwillah R . . . . . . . . . . . . . . . . . . . . . . . . . . . 324
Al Fahmy M . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 49
Al Haifi M . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 308
Al Kharabah AM . . . . . . . . . . . . . . . . . . . . . . . . 329
Al Khulaifi Y . . . . . . . . . . . . . . . . . . . . . . . . . . . . 238
Al Sayegh A . . . . . . . . . . . . . . . . . . . . . . . . . . . . 226
Al Terkait N . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 59
Al-AbdulGhafour SYF . . . . . . . . . . . . . . . . . . . . 311
Al-Ali NS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14
Al-Anazi KA . . . . . . . . . . . . . . . . . . . . . . . . . . . . 214
Al-Anizi F . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 33
Al-Bloushi MAS . . . . . . . . . . . . . . . . . . . . . . . . 315
Al-Einzi LSM . . . . . . . . . . . . . . . . . . . . . . . . . . . 276
Al-Eisa IS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 100
Al-Fadli HAS . . . . . . . . . . . . . . . . . . . . . . . . . . . 118
Al-Faraj JM . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14
Al-Ghareeb H . . . . . . . . . . . . . . . . . . . . . . . . . . . . 28
Al-Hashash W . . . . . . . . . . . . . . . . . . . . . . . . . . 186
Al-Humaidhi A . . . . . . . . . . . . . . . . . . . . . . . . . . 214
Ali JI . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 232
Al-Jady AHA . . . . . . . . . . . . . . . . . . . . . . . . . . . . 118
Al-Jarki FA . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14
Al-Jasem L . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 118
Al-Jassar T . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 100
Al-Jasser AM . . . . . . . . . . . . . . . . . . . . . . . . 171, 214
Al-Kandari MH . . . . . . . . . . . . . . . . . . . . . . . . . 276
Al-Khaldy JA . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14
AlKharji F . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 203
Al-Kussary IMA . . . . . . . . . . . . . . . . . . . . . . . . . 300
Al-Leithy M . . . . . . . . . . . . . . . . . . . . . . . . . . . . .191
Al-Mahmoud NY . . . . . . . . . . . . . . . . . . . . . . . . 284
Al-Maskari M . . . . . . . . . . . . . . . . . . . . . . . . . . . . 10
Al-Mehza AM . . . . . . . . . . . . . . . . . . . . . . . . . . . . 28
Al-Mutairi N . . . . . . . . . . . . . . . . . . . . . . . . . . . . 128
Al-Mutar MS . . . . . . . . . . . . . . . . . . . . . . . . . . . 100
Al-Nakib W . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 21
Alnaqdy A . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 10
Alotaibi S . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 220
Al-Qabandi W . . . . . . . . . . . . . . . . . . . . . . . . . . 241
Al-Qatan HAY . . . . . . . . . . . . . . . . . . . . . . . . . . 220
Al-Qbandi MA . . . . . . . . . . . . . . . . . . . . . . . . . . 292
Al-Rayes M . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 191
AL-Saleh M . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 326
Al-Sanae A . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 241
Al-Saqabi AH . . . . . . . . . . . . . . . . . . . . . . . . . . . . 311
Al-Sawan RMZ . . . . . . . . . . . . . . . . . . . . . . . . . . . 46
Al-Shaibani HI . . . . . . . . . . . . . . . . . . . . . . . . . . 311
Al-Sharkawy IAM . . . . . . . . . . . . . . . . . . . . . . . 147
Alshemmeri N . . . . . . . . . . . . . . . . . . . . . . . . . . 203
Al-Terkit AM . . . . . . . . . . . . . . . . . . . . . . . . . . . 100
Al-Yahya AA . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 28
AL-Zanki S . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 326
Anim JT . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 315
Asadi-Pooya AA . . . . . . . . . . . . . . . . . . . . . . . . . . 25
Aziz S . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 329
Babay HAH . . . . . . . . . . . . . . . . . . . . . . . . . . . . 198
Bader HES . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 207
Baidas G . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 186
Basheer H . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 7
Behbehani JH . . . . . . . . . . . . . . . . . . . . . . . . . . . 141
Bengmark S . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 267
Ben-Nakhi A . . . . . . . . . . . . . . . . . . . . . . . . . . . . 321
Botta GA . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 85
Bourhama MH . . . . . . . . . . . . . . . . . . . . . . . . . . .147
354
Yearly Author Index - Kuwait Medicl Journal (KMJ) 2006; Volume 38
December 2006
Budhdev JA . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 136
Malik SA . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 324
Burud S . . . . . . . . . . . . . . . . . . . . . . . . . . . . 94, 232
Chacko N . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 114
Dashti K . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 321
Davies W . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 3
Devasia A . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 114
Dowod TM . . . . . . . . . . . . . . . . . . . . . . . 43, 94, 232
El Rayes M . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 300
Mapkar OAW . . . . . . . . . . . . . . . . . . . . . . . . 53, 211
El-Din HMA . . . . . . . . . . . . . . . . . . . . . . . . . . . . 122
El-Kishawi A . . . . . . . . . . . . . . . . . . . . . . . . . . . . 138
El-Morshidy AF . . . . . . . . . . . . . . . . . . . . . . . . . . . 7
Fahmy ML . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 191
Fakher O . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 203
George A . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 40
Ghaddar RK . . . . . . . . . . . . . . . . . . . . . . . . . . . . 144
Ghoneim I . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 40
Giacometti L . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 85
Gnanaraj L . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 114
Gopalakrishnan G . . . . . . . . . . . . . . . . . . . . 56, 114
Gupta A . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 136
Gupta B . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 287
Gupta RK . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 229
Habeeb YK . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 315
Hadi I . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 1, 169
Hafez M . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 203
Hammouda A . . . . . . . . . . . . . . . . . . . . . . . . . . . 191
Hashem A . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 43
Hassaniah WF . . . . . . . . . . . . . . . . . . . . . . . . . . 308
Hayat A . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 235
Hegazy AM . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 276
Hegde BM . . . . . . . . . . . . . . . . . . . . . . . . . . . 83, 263
Hussain A . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 321
Ibrahim MK . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 40
Jawad NH . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 241
Johny KV . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 229
Jumaa T . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 308
Kashef S . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 25
Kekre N . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 114
Khallaf F . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 300
Khan AM . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 37
Khan FA . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 133
Lasheen I . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 207
Loutfy SA . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 122
Mahseen SA . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14
Masoud GM . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 118
Mehrabi L . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 203
Moghnai O . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 21
Mohamed MT . . . . . . . . . . . . . . . . . . . . . . . . . . . 332
Mohammed HRA . . . . . . . . . . . . . . . . . . . . . . . . 107
Mukherjee A . . . . . . . . . . . . . . . . . . . . . . . . . . 56, 114
Nadi HM . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 220
Nampoory N . . . . . . . . . . . . . . . . . . . . . . . . . . . . 229
Newman IM . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 107
Oommen MJ . . . . . . . . . . . . . . . . . . . . . . . . . . . . 136
Oudjhane K . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 235
Pacsa A . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 21
Paramasivam RB . . . . . . . . . . . . . . . . . . . . . . . . . 141
Parappil H . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 46
Rabia F . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 7
Radhakrishan SB . . . . . . . . . . . . . . . . . . . . . . . . . 211
Radwan MM . . . . . . . . . . . . . . . . . . . . . . . . . . . .100
Rajaian S . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 56
Rani GR . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 33
Sadak SA . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 59
Senok AC . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 85
Shafik MH . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 332
Shalan YAF . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 220
Sharma PN . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14
Sharma AK . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 128
Sheikh MK . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 133
Shenoy JN . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 238
Shenoy P . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 324
Smallhorn J . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 292
Soni AL . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 46, 138
Suresh CG . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 207
Surrun SK . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 53
Szucs G . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 21
Tamimi DM . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 37
Tayeh R
. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .107
Thrikovil SV . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 138
Uboweja AK . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 141
Vurgese TA . . . . . . . . . . . . . . . . . . . . . . . . . . . 53, 211
Xeroulis GJ . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 3
Yousef TM . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 332
Zubaid M . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 207
December 2006
THE
KUWAIT MEDICAL JOURNAL
Yearly Title Index
Kuwait Medical Journal
(KMJ) 2006; Volume 38
The Kuwait Medical Journal 2006, 38 (4): 355-356
3C Syndrome (Cranio-Cerebello-Cardiac Dysplasia)
Or Ritscher- Schinzel Syndrome: A Rare Case
Report with Review of Literature. 38(2): 138-140.
Comparison of Compliance Versus Non-Compliance
to Anti-hypertensive Agents in Primary Health
Care - An Area Based Study. 38(1): 28-32.
A Novel use of Ureteroscope for a Non-Urological
Cause - A Point of Technique. 38(1): 56-58.
Comparison of Susceptibility Testing Methods for
the Detection of Methicillin/Oxacillin Resistance in
Staphylococcus Aureus. 38(3): 198-202.
A Travel Abroad - Associated Case of Legionella
Pneumonia. 38(1): 59-60.
Accuracy of Axillary Temperature Compared with
Rectal Temperature in Sick Children. 38(1): 25-27.
Adrenal Carcinoma with Cardiac Metastasis in a
Child: Case Report. 38(4): 321-323
Anomalous Coronary Artery from the Opposite
Coronary Sinus in Young Children. 38(4): 292-299.
Antibody Prevalence and Genotype-Specific
Protective Immunity against Mumps Vi ru s
Infection in Children from Kuwait. 38(1): 21-24.
Bacteremia due to Stenotrophomonas Maltophilia
in Patients with Haematological Malignancies.
38(3): 214-219.
Bone Involvement in Hodgkin’s Disease at
Presentation: A Series of Three Case Reports with a
Brief Review. 38(2): 133-135.
Breast Lymphoma: Case Report and Review of
Literature. 38(1): 37-39.
Burned-out Testicular Germ Cell
Mimicking Lymphoma. 38(3): 235-237.
Tumour
Burns and Congenital Indifference to Pain in Two
Sisters: A Case Report. 38(1): 40-42.
Caffey Silverman Disease: Case Report and
Literature Review. 38(1): 49-52.
Carbamezepine Induced Pseudolymphoma. 38(4):
329-331.
Changing Trends in Acute Myocardial Infarction
Management: A Five -Year Study. 38(3): 207-210.
Chronic Pain Clinic in Kuwait: Are We Prepared?
38(3): 169-170.
Computerization in Primary Care: an Insight. 38(4):
311-314.
Congenital Bronchial Atresia: CT- 3D Image
Reconstruction and Virtual Navigation. 38(3): 238240.
Coronary Angiogram is not the Diagnostic Gold
Standard: Plea for Parsimony. 38(2): 83-84.
Dislocation of the Extensor Tendons Over the
Metacarpophalangeal Joints. 38(1): 7-9.
Early Neonatal Hypernatremia with Intraventricular
Hemorrhage - An Unusual Presentation in Two
Cases. 38(1): 46-48.
Early Radiological Results of Femoral Va ru s
Derotation Osteotomy in Spastic Cerebral Palsy.
38(3): 191-197.
Evidence-Based Medicine: Why and How? 38(1): 1-2.
Excision of Ventricular Cysts of Larynx using Zero
Degree and 30 Degree Endoscope. 38(4): 324-325.
Extended-Spectrum Beta-Lactamases (ESBLs): A
Global Problem. 38(3): 171-185.
Factor XIII Deficiency in a Kuwaiti Child. Typical
Presentation with Delayed Diagnosis. 38(2): 147-148.
Factors Influencing Outcome of Congential
Diaphragmatic Hernia. 38(4): 287-291.
Factors Underlying Bottle-feeding Practice in
Kuwait (2001). 38(2): 118-121.
Fatal Case of Systemic Salmonella Infection with
Acute
Renal Failure, Haemolytic-Uraemic
Syndrome and Rhabdomyolisis. 38(3): 229-231.
356
Yearly Title Index – Kuwait Medical Journal (KMJ) 2006 - Volume 38
Feasiblity and Clinical Significance of Echocardiographic Assessment of Aortic Root Compliance in
Hypertensive Patients. 38(4): 276-283.
Frequency and Etiology of Hyponatremia in Adult
Hospitalized Patients in Medical Wards in a
General Hospital in Kuwait. 38(3): 211-213.
Frequency of Thyroid Microsomal and Thyroid
Peroxidase Antibody Levels in a Selected Group of
Omani Patients with Graves Disease. 38(1): 10-13.
Gitelman’s Syndrome: A Separate Disorder or a
Variant of Bartter’s Syndrome. 38(2): 144-146.
Guillain-Barr syndrome in a Patient with RomanoWard Syndrome: A Case Report. 38(1): 53-55.
Hepatitis C Virus Infection in Non-Hodgkin’s
Lymphoma Patients: Virological Evaluation. 38(2):
122-127.
Human Cytomegalovirus Infections in Pregnancy
and the Newborn: Epidemiology, Laboratory
Diagnosis and Medico-Legal Aspects. 38(2): 85-93.
Mirizzi Syndrome: A Review of the Literature.
38(1): 3-6.
Neuronal Ceroid Lipofuscinoses: Report of Five
Cases in Kuwait. 38(4): 315-320.
Osler-Weber-Rendu and Liver Transplant. 38(3):
186-190.
Persistent Narrow Complex Tachycardia; What is
the Diagnosis? 38(3): 226-228.
Plant-derived Health-effects of Turmeric and
Curcomenoids. 38(4): 267-275.
Pretransplant Antitubercular Therapy - How Long?
38(2): 114-117.
Prevalence and Factors Associated with Obesity
and Treatment of Blood Pressure among Kuwaiti
Hypertensive Patients in a Primary Health Care
Clinic. 38(4): 284-286.
Prevalence and Risk Factors for Diabetic Retinopathy
among Kuwaiti Diabetics. 38(3): 203-206.
Prevalence of Osteoporosis and Determinants of
Bone Mineral Density in Healthy CommunityDwelling Kuwaiti Men Aged 50 Years or Older.
38(1): 14-20.
December 2006
Profile of Vitiligo in Farwaniya Region in Kuwait.
38(2): 128-132.
Profound Hyperkalemia and the Electrocardiogram.
Lack of Correlation: A Case Report. 38(3): 232-234.
Results of Combined Proximal Crescentic
Metatarsal Osteotomy and Modified Distal Soft
Tissue Procedure In Severe Hallux Valgus. 38(4):
300-307.
Reversible Posterior Leukoencephalopathy Syndrome:
A Review with Two Illustrative Cases. 38(2): 94-99.
Risk Factors in Acute Poisoning in Children - A
Retrospective Study. 38(1): 33-36.
Safety of Laparoscopy for Acute Cholecystitis.
38(4): 308-310.
Science Versus Scientism. 38(4): 263-266.
Sheesha Smoking among a Sample of Future
Teachers in Kuwait. 38(2): 107-113.
Sickle Cell Intra-Hepatic Cholestasis : A Rare but
Fatal Disease. 38(4): 326-328.
Smoking among Health Care Workers of the
Capital Governorate Health Region, Kuwait:
Prevalence and Attitudes. 38(2): 100-106.
Successful Treatment of Pyogenic Granuloma
Complicating Motility Peg Hydroxyapatite Orbital
Implant Using Topical Steroids Alone - A Case
Report. 38(2): 141-143.
Superior Mesenteric Artery Syndrome: An Uncommon cause of Intestinal Obstruction; Report of Two
Cases and Review of Literature. 38(3): 241-244.
Transient Central Diabetes Insipidus in a Female
Patient with Thrombotic Thrombocytopenic
Purpura and Ectopic Pregnancy: A Possible Link Case Report. 38(1): 43-45.
Unusual Presentation of a Common Disease:
Disseminated Tuberculosis Presenting as Osteomyelitis.
38(2): 136-137.
Urinary Tract Infection in Boys Less Than Five
Years of Age: A General Pediatric Perspective. 38(3):
220-225.
Walker-Warburg Syndrome, A Case Report. 38(4):
332-335.