Download Nutritional Regulation of Gene Expression

Nutrition and Genomics
BMB 505 – Advanced Nutrition and Nutritional
Biochemistry
Yearul Kabir
(Handout # 1)
Date: 09.11.2009
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Nutrition and Genomics
• Nutritional genomics, or nutrigenomics, is the study of how foods
affect the expression of genetic information in an individual and how an
individual’s genetic makeup metabolizes and responds to nutrients and
bioactives.
• Not all individuals respond similarly to food.
• That food alters expression of genetic information and that genotypic
differences result in different metabolic profiles are concepts central to
nutritional genomics – and, indeed, provide the critical link between
diet and health.
• In other words, the need to understand nutritional influence on the
genome and the genome’s influence on metabolism led to the concept
of nutritional genomics.
• The notation that interactions between dietary factors and genes (or
their variants) can promote health or cause disease is perhaps best
captured by the term “nutrigenomics” (a contraction of nutritional
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genomics).
Nutrigenomics
• Nutrigenomics adhere to the following percepts:
• Poor nutrition can be a risk factor for diseases;
• Common dietary chemicals can act on the human genome, either directly
or indirectly, to alter gene expression and/or gene structure;
• The degree to which diet influences the balance between health and disease
depends on an individual’s genetic makeup;
• Some diet-regulated genes (and their common variants) play a role in the
onset, incidence, progression, and/or severity of chronic diseases, and
• Dietary intervention based on knowledge of nutritional requirement,
nutritional status, and genotype can be used to prevent, mitigate, or cure
chronic disease.
• Genomic analysis reveals that humans are 99.9% identical at the DNA
level. This implies that the remaining 0.1% of the human genome (or about
3 million single nucleotide polymorphisms (SNPs) is responsible for all the
morphological, physiological, biochemical and molecular differences
between any two individuals and susceptibility to disease.
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Nutrigenomics …..
• Common genetic variation in the form of SNPs in enzyme-encoding
genes (or their promoters) can affect reaction rates in metabolic
pathways that in turn, can create individual differences in the way we
absorb, metabolize, store, and utilize nutrients.
• SNPs are the most common variation in the primary sequence of
human DNA; more than 10 million SNPs are estimated to be present
in the human genome.
• SNPs are defined as nucleotide base pair differences in the primary
sequence of DNA and can be single base pair insertions, deletions, or
substitutions of one base pair for another.
• SNPs contribute to susceptibility for common disease and
developmental anomalies, and polymorphic alleles have been
identified that increase the risk of common disorders including
neural tube defects, cardiovascular disease, cancers, hypertension,
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and obesity.
Nutrigenomics …..
• The initial successes of nutrigenomics have revealed that indeed the
natural variation in the human genome is responsible for significant
variations in response to diets.
• Therefore, the optimal diet for one individual in a population will
not be the same for every individual in that population.
• As we learn more about the health-promoting dietary chemicals we
eat and how they interact with nutrient-regulated and diseaseassociated genes, we should be able to achieve optimal health and
wellness earlier, maintain it longer, and at a lower cost.
• Just as pharmacogenomics has led to the development of
“personalized drugs,” so will nutrigenomics open the way for
“personalized nutrition”.
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Nutritional Regulation of Gene Expression
• Nutrient regulation of gene expression is a well-recognized topics
in contemporary nutritional science.
• It is difficult to separate direct effects of individual nutrients on
gene expression from those produced indirectly through
physiologically controlled mediators and modulating molecules that
are responsive to the diet.
• The way in which the diet, in concert with hormones, cytokines,
and growth factors, interacts to influence the differential expression
of specific genes has reached such a high level of awareness that a
new term, nutrigenomics has evolved to describe such
phenomenon.
• Nutrigenomics includes all genetic factors, including epigenetic
events, as they modulate individual genes and gene networks.
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Nutritional Regulation of Gene Expression …..
• From the stand-point of nutritional influences on gene expression,
processes are envisioned in which dietary conditions, through either
direct interaction of specific nutrients with transcription factors or
mRNA binding proteins, or, more commonly, through indirect
means (e.g., hormones or signaling systems), produce changes that
define phenotypic expression.
• Classic experiments demonstrated that polyribosome formation
depended on the presence of essential amino acids in the diet.
• In addition, inhibitors of mRNA synthesis (actinomycin D) and
translation (cycloheximide) were used in animal experiments to
study many nutrient-induced changes in gene expression.
• Examples: iron-induced synthesis of ferritin, regulation of
phosphoenolpyruvic-carboxykinase (PEPCK) by high carbohydrate
intake and fasting.
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Your Health – Genes or Environment?
• You have no doubt grown accustomed to thinking about certain
aspects of your physical body, its function and your health as
immutable, given or cast in stone. For example, if you have brown
eyes, you know you will never have blue ones. If you wear size 10
shoes, you will never wear size 6.
• It is Heredity. You inherited your brown eyes.
• However, if genes alone determine the size, shape and function of
our bodies, how can we explain the fact that the average height of
adult Japanese men and women has increased nearly six inches since
WW II?
• The genes have not changed. What has changed is the nutrition of
Japanese children and adolescent.
• Nutritional environment combined with genetic inheritance yields
what is called the “phenotype” of the individual, his or her
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observable size, shape and function.
Disease – Inherited Risk, Not Inevitable Outcome
• Phenotype: The entirephysical, biochemical and physiological
makeup of an individual, as determined both genetically and
environmentally, as opposed to genotype.
• Most people assume that diseases like diabetes, heart disease, high
blood pressure, stroke and cancer are results of genetic inheritance
factors.
• The Human Genome Project is providing that genes are only a part
of the story.
• More important than genetic inheritance is the phenotype – the
result of gene expression and function.
• In terms of your health or disease state as an adult, your phenotype
is determined by the way you have treated your genes throughout
your life.
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Disease – Inherited Risk, Not Inevitable Outcome…
• What you have eaten or drunk, inhaled, surrounded yourself with in
your environment, endured as stresses, participated in as activities
or suffered as injury, infection or inflammation – all of these factors
alter the expression of your genes and contribute in a major way to
your state of health or disease.
• Expression means the way messages that are locked into your
genetic inheritance factors are translated and ultimately influence
your function.
• These changes in function result from two important influences that
modify how your genes are expressed.
• The first is how the messages in your genes are transcribed, and the
second is what happens to the cells of your body after the genes are
translated. (Cell biologists call these “post-translation” effects of
gene expression.)
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Nutritional Modification of Genetic Expression
• In early 1900s, Drs. Joseph and Mary Goldberger research led to
the discovery that nutrition influences gene expression.
• Pellagra: A clinical deficiency due to deficiency of niacin or failure
to convert tryptophan to niacin. It is characterized by dermatitis,
inflammation of mucous membranes, diarrhea and dementia –
psychic disturbances (the 3 Ds of pellagra).
• Each fall and winter in the Southeaster US filled with people with
pellagra. Who contracted pellagra were immigrants from Eastern
Europe; therefore believed to be of genetic origin. The seasonality
of the illness suggested that, like the flu, it was caused by an
infection contracted by genetically susceptible individuals.
• The Goldbergers quickly became convinced from their observations
that pellagra was neither genetic nor caused by the infection.
Instead, they found it resulted from a nutritional deficiency.
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Gene Expression
• During the course of your life, many events alter the way your
genetic characteristics are expressed in individuals cells, tissues or
organs.
• Changes in gene expression may reflect changes in phenotype that
indicate disease or the loss of health and vitality.
• An extreme example of this change in phenotype is the case of J.M.
Barrie, the author of Peter Pan. When he died in his 60s, he was
only 4 feet 10 inches tall and apparently had never gone through
puberty.
• This phenomenon occurred in the absence of any known disease or
genetic abnormality.
• In the medical literature of today, this appears to be a case of
arrested maturation due to a psychological trauma so severe that it
altered gene expression of the hormones required for development.
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Gene Expression….
• Our environment and experiences can play a significant role in
modifying our phenotype. This most remarkable case of streeinduced dwarfism in Barrie demonstrates the power of the
environment to control the activity of our genes.
• In most cases, however, the first manifestation of this type of gene
expression is generally a loss of function that could be as simple as
sleep disturbance, fatigue, chronic pain, changes in body temperature
and weight or poor exercise tolerance.
• These changes may be the early warning signs or what are called
“biomarkers” of altered gene expression. If you do not pay attention
to those early warnings, the result, after many years, could be the
expression of disease.
• Physical fitness improves your health. Exercise is good for you.
• The complete explanation is that moderate regular exercise is one of
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the factors that improves gene expression and alters your phenotype.
Can Food Improve the Expression of Our Genes?
• One meal does not make a difference in the expression of your
genes, but over the course of many years your dietary choices can
influence your gene expression in such a way as to modify your
phenotype, enhancing or diminishing your cellular function.
• This does not mean that food changes your genes in any way. The
message you were born with remains intact, embedded in the
nucleus of cells in every organ of your body.
• What does change is the way the message from your genes is
expressed.
• The effect of the nutrients you ingest on the expression of messages
within your genes is like the effect of hydroxyurea or butyrate on
sickel cell anemia.
• Both substance are capable of waking up the sleeping message in
the genome for the production of fetal hemoglobin.
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Figure: Red-Cell Sickling
•
Sickel cell anemia a “molecular disease” because just one molecule was damaged due to a
genetic uniqueness (i.e., a genetic mutation).
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Can Food Improve the Expression….
• When a fetus is in the womb, its hemoglobin is unique in its
structure and ability to capture oxygen from the mother’s blood
supply.
• After birth, the genetic message for the production of this type of
hemoglobin goes to sleep and is replaced by the message for the
production of adult hemoglobin.
• The fetal hemoglobin message is still on the genome; it is just not
being expressed.
• Administering hydroxyurea or butyrate to an individual who carries
the genetic message for the production of sickle hemoglobin
awakens the message to produce the normal fetal hemoglobin that
dilutes the sickel hemoglobin, preventing it from crystallizing.
• This nutritional intervention is a classic example of the genetic
nutritioneering approach.
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Can Food Improve the Expression….
• By using a substance that modifies genetic expression, it is
possible to alter the course of a genetically determined illness.
• Genetic messages can either be put to sleep or awakened as a
consequence of alterations in your diet. Putting to sleep the
messages that result in increased risk of disease and awakening
those messages enhance health.
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How diet Influences Genetic Expression
• The understanding that diet can modify gene expression achieved
a new level of acceptance due to the pioneering work of Michael
Brown & Joseph Goldstein on cholesterol and its relationship to
heart disease.
• They found that there is a basic defect (genetic trail) in families
whose members have high incidence of heart disease, which is
associated with very high blood cholesterol levels. That genetic
trail occurs in about 1 in 500 individuals worldwide.
• Affected individuals have elevated blood levels of the “bad” LDL
cholesterol. Over time, cholesterol is deposited in arteries,
resulting in plaque and a narrowing of the arteries which leads to
heart disease, particularly in males with this genetic condition who
are between the ages 35 and 50.
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How diet Influences Genetic Expression….
• In these individuals the difficulty is not necessarily that they are
consuming too much cholesterol in their diet. Instead, their bodies
produce too much cholesterol as a consequence of a defect in the
thermostat that regulates the manufacture of choleterol in the liver.
• Through their pioneering work, statin drugs were found that could
turn off the thermostat that controls cholesterol synthesis.
• The result was a reduction in cholesterol and in heart disease
incidence among these individuals.
• Significant side effects, including a potential increased risk of
cancer, have subsequently been associated with these cholesterollowering drugs in some individuals.
• A number of recently discovered dietary substances can also help
regulate the cholesterol thermostat. One such substance is
tocotrienol, a nutrient found in high levels in rice, barely and palm
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oils.
How diet Influences Genetic Expression….
• This is one example of a specific food that is enriched in a certain
nutrient that can have an impact on physiological function in
individuals with specific genetic risk.
• Research has also been conducted into the management of high
blood pressure with nutritional modulation of gene expression and
function. Increased intake of fresh juices of fruits and vegetables
rich in potassium and magnesium, along with calcium
supplementation, has been found helpful in lowering blood pressure
in individuals with essential hypertension who have not responded
to sodium restriction.
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Phytochemicals and Gene Expression
• Phytochemicals are plant-derived substances that can modify gene
expression or physiological functions in individuals who consume
them.
• One example of the power of phytochemicals is the recent report
that the flavonoid naringenin, which is found in grapefruit but not
in orange, lemon or lime, can assist the costly prescription drug
cyclosporin in preventing organ transplant rejection after surgery.
• Naringenin suppresses the gene expression for a detoxifying
enzymes in the liver that eliminates the drug cyclosporin from the
body. By inhibiting the expression of this enzyme, naringenin helps
patients get more benefit from cyclosporin by preventing its
detoxification, thereby slowing its elimination from the body.
• A number of biologically active substances in foods help regulate
gene expression.
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Phytochemicals and Gene Expression….
• Limonene, a monoterpene nutrient found in grapefruit and
orange juice, inhibits tumor formation by stimulating the gene
expression for a detoxifying enzyme called glutathione Stransferase. Glutathione S-transferase is an important enzyme
that promotes the detoxification of cancer-producing chemicals
and their elimination from the body as nontoxic derivatives.
• Garlic is another food that contains a number of phytochemicals
that can help modulate gene expression. The sulfur compounds
in garlic help protect against carcinogenic chemicals, lower blood
pressure and blood cholesterol levels and help boost immunity.
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Vitamins, Minerals and Gene Expression
• Vitamin B6 (pyridoxine), vitamin B12 (cobalamin) and folic acid
play important roles in modulating gene activity through their
ability to mask certain portions of the gene that should not be
expressed in adults. Through this masking effect, messages related
to the risk of both heart disease and cancer can be put to sleep.
• The essential trace mineral zinc is important in modulating gene
expression as well.
• Zinc is a pivotal nutrient in supporting immune system function and
it helps regulate the way that the genetic message is translated into
protein synthesis in the cell.
• One of the first signs of zinc inadequacy is the loss of taste or
smell.
• Individuals whose gene expression is modified as a consequence of
zinc insufficiency frequently have a poor sense of taste or smell.
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Foods and Gene Expression
• Scientists have learned during the past decade that the nutrients
found in foods engage in complex interactions with our genetic
machinery.
• Your food and beverage selections play a significant role in
determining aspects of your gene expression.
• Each of us carries different genetic sensitivities to nutrients, and
therefore, a diet that may be optimal for someone else may not even
be adequate for you.
• Over the course of the lifetime of an individual food substances
may be much more important in determining health and disease
patterns than the drugs he or she may take for a short period of
time.
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Foods and Gene Expression
• Genes affect our response to the food we eat on several levels. They
influence the way we absorb, metabolize, and excrete nutrients.
• They partially control other factors, such as taste and smell, and
how quickly or slowly we feel full after eating a meal.
• For example, phenylthiocarbamide (PTC) crystals taste bitter to
some people and not to others because genes control the ability to
taste this substance. Those who can taste PTC show a greater
sensitivity to bitterness in other substances, such as saccharin and
caffeine, and to the sweetness of sugar.
• They also can detect the sharp taste of cruciferous vegetables and
dislike cabbage, brussels sprouts, and broccoli.
• This indicates once more how important individual reactions are.
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How Our Diet Communicates with Our Genes
• The exposure of your genotype to specific foods, stress, and environmental
and lifestyle factors, such as smoking and alcohol consumption, result in
altered function of your genotype as expressed in your phenotype.
• Certain genetic characteristics can be induced by exposure to specific foods
and nutrients, and other genetic characteristics may be suppressed.
• The communication between the food you eat and your genotype
contributes to your health by modifying your phenotype or function.
• For example, oat bran or wheat bran will or will not help to lower a
person’s blood cholesterol level depends on that person’s genes.
• The individuals whose cholesterol goes down in response to increased
dietary fiber are those who are carriers of two particular gene variants. One
is the E2 allele; the second is a change in the base pair at a specific site of
the low-density lipoprotein receptor (LDLR).
• A genetic test can therefore determine who will lower his or her blood
cholesterol by eating more fiber, and who will not. It is clear that future
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nutritional advice will be based on each individual’s genotype.
How Our Diet Communicates with Our Genes….
• Sugar Sensitivity
• Researcher has found that many individuals have experience
serious digestive problems or disorder, including colitis, irritable
bowel syndrome (IBS) and Crohn’s disease due to carbohydre diet.
• How could the carbohydrate in foods lead to serious digestive
inflammation and ulceration?
• One answer that is emerging from research is that individuals with
specific genetic inheritance factors are more sensitive to fructose.
• There are a variety of genetic uniquenesses in the way that
individuals metabolize sugar and absorb it from their intestinal
tract.
• Fructose sensitivity, which results from the altered absorption and
metabolism of fructose, can result in inflammation of the intestinal
tract.
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How Our Diet Communicates with Our Genes….
• Another sugar that produces digestive difficulty in individuals with
specific genetic inheritance factors is the milk sugar lactose.
• Individuals who complain of diarrhea, gas and intestinal pain after
drinking milk may suffer from the genetic inheritance of lactose
intolerance.
• Some people have a genetic sensitivity not to milk sugar but to the
milk protein casein.
• Some genetic characteristics are “constitutional,” which means the
expression of the genes that encode for these characteristics is not
easily modified by changes in diet, lifestyle or environment.
• Other genetic characteristics, however, are inducible: their
expression can be activated or suppressed by dietary, environmental
or lifestyle exposures. Inducible genetic characteristics, which are
sensitive to what you eat, form the basis of the genetic
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nutritioneering approach.
Detoxification, Genotypes and the Risk of Disease
• Alcohol consumption provide an illustration of the inducible nature
of the genes. At the modest levels of intake, alcohol is metabolized
in the liver by action of the enzyme alcohol dehydrogenase.
• At high levels of intake the genes are induced to express a different
detoxification enzyme (i.e., cytochrome P450 1e2), which, in its
alcohol-metabolizing activity, releases oxidants that can damage the
liver.
• Liver damage that is observed as a result of excessive alcohol
intake is caused in part by this inducible factor from altered gene
expression.
• A person can defend him/herself against the damaging effects of
oxidants released after alcohol consumption by increasing his or her
dietary intake of antioxidants like vitamin E, thereby providing
protection against this inducible process.
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Detoxification, Genotypes and the Risk of Disease….
• Scientists have identified specific genotypes that have a higher risk
of certain diseases as a consequence of reduced detoxification
ability.
• Cigarette smokers who carry in their genes poor detoxification may
have a more toxic response and a greater cancer risk from smoking
than those who got the genetic luck of the draw and have better
detoxification ability.
• A study of breast cancer in women found a much higher incidence
of breast cancer in smokers who had very poor detoxification
ability as a consequence of the poor genetic expression of a
detoxification enzyme called N-acetyltransferase (NAT).
• Similarly, lung cancer risk in smokers is increased in individuals
who have a genetically sluggish detoxifacation enzyme called
glutathione transferase.
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Detoxification, Genotypes and the Risk of Disease….
• A single exposure or a single substance may not overburden the
body and induce damage. It is the total exposure to toxic substances
and how effectively they can be detoxified that determines relative
health risk.
• A man who lives in a very polluted environment, pursues an
occupation that exposes him to toxic substances, smoke cigarettes,
drinks excessive alcohol, has a poor-quality diet and eats foods like
charbroiled meats that are high in toxic substances adds constantly
to the total load on his detoxification machinery. Eventually, it can
be overwhelmed.
• If he has a sluggish detoxification system as a consequence of
specific genetic uniqueness, he definitely becomes a potential
candidate for heart disease, cancer, arthritis or neurological disease.
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Detoxification, Genotypes and the Risk of Disease….
• The medical and scientific communities now recognize that diet
plays an important role in modifying detoxification ability.
• Poor-quality diets that are very high in toxic substances and low in
nutrients that help support gene expression of detoxification
enzymes result in increased risk of toxic reactions.
• Diets that are low in toxic substances and high in the nutrients that
support the expression of inducible genes associated with
detoxification, on the other hand, can make individuals much more
tolerant of exposure to various toxins.
• One of the first studies that indicated the important role of dietary
substances in modifying detoxification ability occurred in 1945,
when investigators reported that detoxification of caffeine-like
substances could be enhanced by specific dietary factors.
• These dietary factors included increased levels of protein, adequate levels of
the B vitamins, improved antioxidant intake and proper mineral nutrition.
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The Genetic Impact
• It is important to distinguish between the genetic and nongenetic
forms of hyperlipidemia.
• Individuals with the genetic form will experience severe high blood
cholesterol, sometimes in the 400 to 600 mg/dl range, because of a
genetic defect in the way the body handle, or metabolizes,
cholesterol. Often this occurs because they do not have enough LDL
receptors, allowing excessive amounts of LDL to circulate in the
blood.
• Their serum cholesterol will be high despite normal or low amounts
of cholesterol and saturated fat in their diets.
• Therefore, doctors must use drugs to treat this type of hyperlipidemia
– because diet and other lifestyle changes are simply inadequate to
reduce serum cholesterol levels.
• The presumed nongenetic form of hyperlipidemia is much more
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common.
The Genetic Impact
• It is important to distinguish between the genetic and nongenetic
forms of hyperlipidemia.
• Individuals with the genetic form will experience severe high blood
cholesterol, sometimes in the 400 to 600 mg/dl range, because of a
genetic defect in the way the body handle, or metabolizes,
cholesterol. Often this occurs because they do not have enough LDL
receptors, allowing excessive amounts of LDL to circulate in the
blood.
• Their serum cholesterol will be high despite normal or low amounts
of cholesterol and saturated fat in their diets.
• Therefore, doctors must use drugs to treat this type of hyperlipidemia
– because diet and other lifestyle changes are simply inadequate to
reduce serum cholesterol levels.
• The presumed nongenetic form of hyperlipidemia is much more
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common.
The Genetic Impact….
• Here the individual’s genoptype is normal, but detrimental lifestyle
factors – being obese, leading a sedentary lifestyle, and consuming a
diet that is high in cholesterol and saturated fat for many years –
raise blood cholesterol levels above the 200-240 range.
• This diet induced high cholesterol is one situation where dietary
changes, such as eating less fat and more fish, and other lifestyle
changes, including regular exercise and weight loss, can make a
difference.
• Such dietary and behavioral modifications can lower the levels of
total blood cholesterol, HDL, LDL, and triglycerides.
• Recent research shows that more and more of the risk factors for
coronary heart disease are caused by genes. In addition to
abnormalities in LDL receptor activity, faulty genes may produce
low HDL cholesterol levels and affect blood pressure, a person’s
insulin level and his or her insulin response.
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Familial Hypercholesterolemia (FH)
• This disorder, which afflicts 15 percent of those with heart
attacks, occurs because of a mutation in a single gene that leads to
unusually high blood levels of cholesterol and premature
development of atherosclerosis.
• Individuals with only one mutant gene develop the condition
because this is an autosomal-dominant trait in which the defective
gene overpowers the normal gene of handling cholesterol.
• Although they are not obese, people with FH experience two to
three times the average level of blood cholesterol at birth, and the
condition persists throughout life.
• About 10% of those with one mutant FH gene have elevated
triglyceride levels as well.
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Familial Hypercholesterolemia (FH)….
• Since there are more than 100 different mutations, they collectively
affect 1 in every 500 people in the USA, making familial
hypercholesterolemia the most common disorder caused by a single
abnormal gene.
• The basic defect here is in the gene that is found on the cell surface
of the LDL receptor, located on chromosome 19.
• The cell produces only half the number of receptors that remove
LDL cholesterol from the blood, causing a cascade of ill effects –
high blood cholesterol levels, cholesterol deposits in the arteries, and
the consequent arterial blockages that produce coronary heart disease
early in life.
• Men experience problems as young as their thirties or forties, with
an average age of forty-three at the first heart attack; for women this
occurs ten years later.
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Familial Hypertriglyceridemia
• This condition, responsible for 5% of heart attacks, is common in the
US population.
• 10% of men between the ages of 35 and 39 have triglyceride levels
above 250 mg/dl.
• It is also an autosomal-dominant disorder that shows up in early
childhood or at puberty.
• The underlying defect here is a single faulty gene that increases the
production of triglycerides in very low density lipoproteins
(VLDLs), decreases their breakdown, and produces an accumulation
of triglycerides in the blood.
• Typical levels are in the 200 to 500 mg/dl range, particularly in
people who eat high carbohydrate diets.
• These patients are usually obese, have high blood pressure, and have
high levels of sugar, insulin, and uric acid in their blood.
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Genes, Diet, and Cardiovascular Disease
• Dyslipidemia is commonly associated with the development of
atherosclerosis and can be caused by improper function of a variety
of proteins that control lipid homeostasis, such as nuclear factors,
binding proteins, apolipoproteins, enzymes, lipoprotein receptors,
and hormones.
• Polymorphisms have been identified in most of these components
and many of the underlying genes have been explored in terms of
diet–gene interactions.
• Amongst these, the apolipoprotein E gene (apoE) is the most
intensively studied with regard to its effects on low-density
lipoprotein (LDL)-cholesterol levels in response to dietary
interventions.
• Genetic variation at the apoE locus results from three common
alleles in the population, E4, E3, and E2. However, other genetic
variants at the apoE locus have been described as well.
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Genes, Diet, and Cardiovascular Disease …..
• Besides the fact that LDL-cholesterol levels were highest in
subjects carrying the apoE4 isoform, this association was
especially prominent in populations consuming diets rich in
saturated fats and cholesterol.
• These epidemiology data, therefore, indicate that high LDLcholesterol levels are manifested primarily in the presence of an
atherogenic diet but that an individual’s response to dietary
saturated fat and cholesterol may differ depending on the
individual apoE alleles.
• However, it needs to be stressed that especially for apoE,
investigations of diet–gene interactions have yielded quite diverse
outcomes.
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Genes, Diet, and Cardiovascular Disease …..
• Significant diet–apoE interactions occurred in studies focusing on
males, suggesting a significant gene–gender interaction.
• Baseline lipid levels seem to affect the outcome and significant
associations were frequently found only in subjects who were
moderately hypercholesterolemic.
• More consistent effects were reported on the impact of alcohol intake
on LDL-cholesterol depending on the apoE genotype in men.
• A negative association between alcohol consumption and LDLcholesterol was found for carriers of apoE2, whereas subjects with
apoE4 displayed a positive correlation.
• Within these genotype studies apoA1 has emerged as a primary
candidate for genetic variability in high-density lipoprotein (HDL)
levels and its gene product plays a crucial role in lipid metabolism
and for cardiovascular disease risk.
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Genes, Diet, and Cardiovascular Disease …..
• In women it has been found that a G to A transition in the apoA1
gene is associated with an increase in HDL-cholesterol levels
depending on the dietary intake of polyunsaturated fatty acids.
• Similar to this G/A single-nucleotide polymorphism in apoA1,
increased HDL levels were found to be associated with a
homozygous 514(CC) polymorphism in the hepatic lipase gene in
response to higher fat contents in the diet.
• This increase in the level of protective HDL particles was interpreted
as a defense mechanism that was not found in subjects carrying the
TT genotype.
• Interestingly the TT genotype is common in certain ethnic groups,
such as African-Americans, and might help to explain their limited
ability to adapt rapidly to new nutritional environments.
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Gene Regulation by Nutrients
• Regulation of gene expression by nutrients.
• A ‘direct’ effect of some nutrients (vitamin A, D, and E; zinc; n-3
fatty acids; and sterols) on gene transcription is shown in which,
subsequent to ligand binding to a specific transcription factor,
cytoplasmic to nuclear translocation of the complex occur, and
interaction through a specific domain of the factor with a response
element sequence (specific nucleotide sequence) of the regulatory
region produces a change in transcription rate of the gene.
• Some nutrients activate transmembrane receptors, which use
intracellular signaling pathways to initiate or modify gene
expression.
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Gene Regulation by Nutrients
• Regulation of gene expression by nutrients.
• A ‘direct’ effect of some nutrients (vitamin A, D, and E; zinc; n-3
fatty acids; and sterols) on gene transcription is shown in which,
subsequent to ligand binding to a specific transcription factor,
cytoplasmic to nuclear translocation of the complex occur, and
interaction through a specific domain of the factor with a response
element sequence (specific nucleotide sequence) of the regulatory
region produces a change in transcription rate of the gene.
• Some nutrients activate transmembrane receptors, which use
intracellular signaling pathways to initiate or modify gene
expression.
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Regulation of gene expression by nutrients …..
• Single nucleotide polymorphisms and epigenetic changes can
modify the expression of some gene.
• Nutrient effects on mRNA processing, editing, stability, and
translation have been documented.
• Nutrients which have a direct effect on gene transcription include
vitamin A (retinoic acid), vitamin D (calcitriol), zinc, n-3
polyunsaturated fatty acids, and specific sterols.
• In contrast, iron, and perhaps other nutrients, has a direct effect
on gene regulation through control of translation or stability of
specific mRNA.
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Regulation of gene expression by nutrients..
• Frequently, gene regulation by nutrients is more complex, where
multiple and interconnected factors, including nutrient effects on
signal transduction pathway, epigenetic effects on specific genes,
mRNA splicing and translation, and posttranslational modifications,
merge to define indirect effects on expression of a specific gene.
• Although the primary focus of nutritional genomics is the
understanding of nutrient-gene interactions, expression of genetic
information also is influenced by numerous environmental factors.
• For example, cytokine levels are unusually sensitive to
environmental changes and serve as good markers of environmental
influences that may alter protein and RNA expression.
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Examples
• Some examples of non-nutrient environmental factors affecting
cytokine concentrations are:
• Overall sleep time and sleep continuity.
• Oxygen tension, which is related to altitude.
• Over-the-counter drugs (nonsteroidal anti-inflammatory drugs).
• Water intake relative to tea and other beverages.
• Psychological factors like stress.
• Exposure to allergens and pollutants.
• Balance between energy intake and expenditure.
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Genotype – Environment Interactions
• Genes that cause chronic diseases must be regulated directly or
indirectly by calorie intake and/or by specific chemicals in the diet
because diet alters disease incidence and severity.
• The progressive and sometimes slow change in phenotype from
health to disease must occur, at least in part, through changes in gene
expression.
• These are gene-environment interactions.
• The precise, statistical definition of gene-environment interaction is
“a different effect of an environment exposure on disease risk in
persons with different genotypes” or, alternatively, “a different effect
of a genotype on disease risk in persons with different environmental
exposures”.
• In other words, nutrients affect expression of genetic information and
genetic makeup affects how nutrients are metabolized.
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Genotype – Environment Interactions …..
• A dietary chemical or its metabolite may alter the expression of a
susceptibility gene or its variant that in turn affects other genegene interactions.
• The consequence of such gene-environment interactions may not
only be apparent on the gene of interest, but may also affect the
action of that gene on other interacting genes.
• Different functional classes of genes may have greater importance
than others: affecting the expression of a nuclear receptor or
signal transduction pathways may affect more processes than
altering the expression of a gene encoding an enzyme in a
metabolic pathway.
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Genotype – Environment Interactions …..
• In the short term, the environment almost never improves genes by
changing the DNA sequence; however, the control of genes can be
changed, and potentially improved, by modulating epigenetics and
early development through diet.
• Epigenetic changes are those heritable changes in gene expression
that do not require changes in DNA sequence.
• These usually involve enzymatic DNA methylation and concomitant
changes in histone modifications, such as methylation and
acetylation, and in other modifications of chromatin structure.
• Many effects are considered epigenetic if, without mutation, they
change the long-term physiological, metabolic, or anatomical state of
plants or animals even if the specific gene expression has not been
identified.
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Example: Phenotype – Environment Interactions
• Phenotype to show genotypic differences.
• Individuals with small, dense LDL particles (phenotype B) have an
increased risk of coronary artery disease relative to those individuals
exhibiting large, less dense LDL particles (phenotype A).
• The expression of phenotype A depended on diet: 12 out of 38 men
who switched from a 32% fat diet to a diet containing 10% fat
developed the phenotype B pattern.
• Al least three distinct genotypes were present in this group, one
genotype each for the A or B phenotype and a third genotype that is
responsive to low fat/high carbohydrate diets.
• This genotype produces the A phenotype when these individuals eat
a diet containing 32% fat, but a B phenotype when fed 10% fat – a
result that can be explained by genotype – environment interactions.
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Phenotype – Environment Interactions …..
• Although much attention in the nutrigenomics community is focused
on gene regulation by dietary factors, dietary chemicals also alter the
activity of proteins and enzymes directly.
• Mutations or polymorphisms in genes often result in the
corresponding enzymes having an increased Km (michaelis constant)
for a coenzyme.
• The Km is a measure of affinity of ligand for its protein. Increases in
Km result in decreased affinity of coenzyme and therefore enzymes
with increased Km have a decreased activity.
• Increasing the concentration of the coenzyme, which may come from
diet, can ameliorate the effect of the decreased Km.
• This concept is called the Km constant and is an example of how
alterations in diet may influence individuals differently depending on
their genetic makeup.
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Common Genetic Variants and Gene-Diet
Interactions: Example
• A classical example of gene-diet statistical interaction is between the
-75A/G polymorphism of the apolipoprotein A-I gene (APOAI) and
polyunsaturated fatty acid (PUFA) intake.
• In women – a statistical significant gene-diet interaction (p < 0.05)
was found between PUFA intake as a three category variable (<4%
of energy from fat, 4-8%, and >8%) and the APOAI SNP in
determining plasma HDL-C concentrations.
• This interaction shows that PUFA intake clearly modulate the effect
of -75A/G polymorphism on HDL-C concentrations.
• Thus, in carriers of the A allele, higher PUFA intakes were
associated with higher HDL cholesterol concentrations, whereas the
opposite effect was observed in G/G homozygotes.
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Gene-Diet Interactions: Example
• The Pro12Ala polymorphism in the peroxisome proliferators
activated receptor γ (PPARγ) gene has been associated with a
decreased risk of T2DM (Type 2 diabetes mellitus).
• PPARγ is activated by specific fatty acids and is a master regulator
of adipocyte differentiation.
• One study reported an interaction with the Pro12Ala polymorphism
and the polyunsaturated fat to saturated fat (P:S) ratio of the diet. It
has been found that in carriers of the Ala allele (both heterozygotes
and homozygotes), there was a negative association with the P:S
ratio and fasting insulin, but only in physically active subjects and
not sedentary subjects.
• Another study reported an inverse relationship between BMI and
monounsaturated fat intake in Ala carriers, but not Pro homozygotes.
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Dietary Regulation of Mammalian
Fatty Acid Synthase Gene
• The rate of fatty acid biosynthesis is primarily determined by the
availability of glucose. Consuming a diet rich in carbohydrate
elevates circulating glucose, which in turn signals the secretion of
hormones which effect de novo synthesis of fatty acids.
• Among these hormones, insulin and thyroid hormone (T3) are
increased, and glucagon is decreased. Conversely, glucagon is
decreased during feeding and elevated during starvation.
• Glucose, insulin, T3, and angiotensin II stimulate fatty acid synthesis
and the expression of the fatty acid synthase gene while glucagon
and PUFA downregulated FAS gene expression.
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The mechanisms of regulation of fatty acid synthase by the
nutritional and hormonal factors
• Several transcription factors, which bind specific cis-acting response
elements in the FAS gene, mediate its dietary and hormonal
regulation.
• The cis-acting elements necessary for tissue-specific, nutritional, and
hormonal regulation of FAS expression were identified using
transgenic mice expressing FAS promoter linked to the
chloramphenical acetyltransferase (CAT) reporter gene.
• There is strong positive correlation between mRNA levels and the
tissue-specific gene expression patterns of the reporter and the
endogenous FAS in transgenic mice.
• Fasting and refeeding, insulin and glucocorticoids regulated
expression of the reported gene and the endogenous FAS gene in a
similar manner. In contrast, PUFAs dramatically suppressed
endogenous FAS mRNA in transgenic mice compared to those fed
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oleic acid.
In vivo Effects of Fasting, Refeeding, and Aging
• Fasting decreased conversion of glucose into fatty acids; when these
animals are subsequently refed a low-fat, high-carbohydrate diet
there is a rapid and efficient increase in production of fatty acids and
triglycerides.
• Such changes are mediated by hormonal changes in response to diet.
• Feeding a high-carbohydrate diet is accompanied by an increase in
circulating insulin levels, which increase the transcriptional rate of
fatty acid synthase, as well as other lipogenic genes.
• While FAS mRNA was dramatically and rapidly induced by fat-free
diets in young rats, this response was much slower in aged rats. In
addition to delaying transcriptional activation, maximum rates of
gene transcription were not achieved until animals had been
maintained on a fat-free diet for 24 h. This implies that aging is a
factor in the regulation of lipogenic gene transcription.
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Effects of Insulin
• FAS mRNA is low in animals made insulinopenic by
administration of streptozotocin (STZ), a pancreatic β-cell toxin,
compared to untreated animals. This effect is countered by insulin
administration.
• Insulin treatment results in the rapid induction of FAS mRNA and
gene transcription. Within 6 h of insulin administration to STZtreated animals, FAS mRNA levels were induced to a level
comparable to that observed when refeeding a low-fat, highcarbohydrate diet to previously fasted normal mice.
• Cyclohexamide, an inhibitor of protein synthesis, completely
abolished the effect of insulin, demonstrating that transcriptional
regulation of FAS by insulin requires ongoing protein synthesis.
• Insulin is the most extensively studied and best understood
regulator of FAS gene expression.
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Regulatory Effects of PUFA
• PUFA are known to suppress hepatic mRNA levels in several
lipogenic genes, including FAS. With the exception of glucose-6phosphate dehydrogenase, PUFAs exert their regulatory effects at
the level of transcription.
• PUFAs exert dominant negative effects on many of the genes of
lipogenesis and known to override the stimulatory effects of insulin,
carbohydrates, and thyroid hormones.
• Furthermore, the direct effects of PUFAs on the liver do not require
extrahepatic factors.
• PUFAs are known to suppress hepatic gene expression through three
distinct pathways:
– A peroxisome proliferator activated receptor (PPAR)-dependent pathway,
– A prostanoid pathway, and
– A PPAR and prostanoid-independent pathway.
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Regulatory Effects of PUFA …..
• Feeding PUFA resulted in a decrease in the mature form of SREBP1 in liver nuclei.
• Studies using transgenic mice confirmed that the suppressive effect
of PUFAs on hepatic FAS expression is due to a decrease in the
mature form of SREBP-1 protein.
• The suppressive effects of dietary PUFAs on SREBP-1 expression
mediate the subsequent regulation of FAS expression.
• This has been confirmed by feeding fish oils, which downregulate
the mature form of SREBP by decreasing SREBP-1c mRNA
expression and leads to the concomitant decrease in hepatic FAS
mRNA.
• Studies using cultured hepatocytes linked fatty acid peroxidation to
the effects of PUFAs on gene expression. These findings suggest that
the in vivo inhibitory effects of PUFAs on lipogenic genes could be
mediated indirectly by a peroxidative mechanism.
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Regulatory Effects of Thyroid Hormones
• Thyroid hormone (T3) is elevated during refeeding of fasted animals.
• Thyroid hormone stimulates FAS expression through a mechanism
that is independent of insulin.
• Administration of thyroid hormone to rats for 7 days doubled FAS
activity in liver. Furthermore, hypothyroidism reduced hepatic FAS
activity.
• Increase in FAS activity is due to an increase in gene transcription
and is accompanied by an increase in FAS mRNA.
• Thyroid hormone exerts its effects on FAS transcription by
heterodimerization of ligand-bound thyroid hormone receptor (TR)
with the retinoid receptor, RXR.
• The TR/RXR heterodimer binds to the consensus thyroid hormone
response element (TRE) and promotes gene transcription.
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Regulatory of the FAS Gene by Other Nutrients
• Other nutrients, including dietary protein and minerals, regulate
FAS gene expression.
• Hepatic FAS mRNA abundance in fatty rats was significantly
lower after feeding soybean protein compared to feeding casein.
• The regulation of FAS by essential amino acids was also reported
in HepG2 cells.
• A deficiency of dietary copper is accompanied by a 2-fold
increase in hepatic fatty-acid biosynthesis. Dietary copper
deficiency was demonstrated to increase hepatic FAS activity
associated with a reduction in gene transcription.
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Regulation of SCD Expression by PUFA
• PUFA have been shown to reduce the expression of Stearoyl-CoA
desaturase (SCD) and many enzymes involved in lipid and
carbohydrate metabolism.
• By reducing the expression of these enzymes, it is believed that
PUFAs control the de novo synthesis of saturated, monounsaturated,
and polyunsaturated fatty acids.
• Only when the animal ingests carbohydrate over and above its
energy requirements is the repressive effect of PUFAs overcome and
the lipogenic enzymes induced.
• The regulation of SCD by PUFAs may occur at several levels.
Mainly at the level of SCD gene expression.
• The repression of SCD gene expression by PUFAs is not liver
specific.
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Regulation of SCD Expression by PUFA ….
• Many mechanisms may exist for regulating the tissue-specific of
the SCD genes by PUFAs but recent investigationa show that
PUFAs repress the SCD gene expression mainly at the level of
gene transcription and mRNA stability.
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Epigenetics and Nutrition can Greatly Modulate
Genetic Predispositions
• Well-defined genetic diseases of metabolism (e.g., inborn errors of
metabolism that may be fatal in childhood) often point the way to
discovery of alleles whose effects are less severe but that
nevertheless take a heavy toll over time (over decades) or during
pregnancy.
• These may be greatly exacerbated by nutritional deficiencies that
would not necessarily affect a normal person or animal. These
less severe versions of genetic diseases may be heterozygous
(just one copy of a null or defective gene) or homozygous (such
as two copies of a gene whose products are functional but have
low enzymatic activity due to poor binding of cofactors).
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Epigenetics and Nutrition…
• In human homocysteinuria, methyl metabolism is severely
compromised, often due to homozygous null mutations in a key enzyme
such as cystathionine-beta-synthetase (CBS) or methylenetetrahydrofolate reductase (MTHFR).
• In spite of this, homocysteinuria can be substantially controlled, and
patient health and survival vastly improved, using nutrient balances that
allow the genetic and enzymatic deficiencies to be bypassed in
alternative pathways.
• Similarly, alleles with just moderate differences in activity, at least with
relation to plasma homocysteine (HCY) levels, can be largely or
entirely compensated by increasing folate and/or betaine in the diet.
• These same nutrients are important for maternal nutrition to avoid
neural tube birth defects as well as, potentially, for adult nutrition to
avoid cardiovascular disease and dementia.
• Thus, in many cases, genetic “predisposition” to certain diseases can be
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obviated by a diet specific to genotype.
Nutrigenetics – Examples and Limitations
• Nutrigenetics aims to understand the effect of genetic variations on
the interaction between the diet and disease or on nutrient
requirement. Consequently the major goal is to identify and
characterize gene variants associated or responsible for differential
responses to nutritional factors.
• In the final stage, nutrigenetics could provide the rationale for
recommendations regarding the risks and benefits of a particular diet
or dietary components based on the individual’s genetic makeup.
• Although the methods for detecting single-nucleotide
polymorphisms (SNPs) or haplotypes are improved constantly,
phenotype analysis and assigning alterations in protein functions to
an SNP or haplotype is going to be the pinhole.
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Nutrigenetics – Examples and Limitations …..
• Although mostly inconclusive, preliminary results involving
gene–diet interactions for cardiovascular diseases and cancer
suggest that the concept could work and that we will be able to
harness the information contained in our genome.
• Most of the available data are derived from molecular
epidemiology studies. As all multifactorial nutrition-dependent
diseases require a long period of exposure to the same or similar
dietary patterns to develop a disease, phenotype epidemiological
studies are the tool of choice to assess genetic variation and
disease development or progression.
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Recommende Books
• Genetic – Nutritioneering By Jeffrey S. Bland
• Nutritional Genomics Edited by Jim Kaput and Raymond L.
Rodriguez
• Genetic Nutrition By A. P. Simopoulos, Victor Herbert and Beverly
Jacobson
• Nutrient-Gene Interactions in Health and Disease Edited by Naima
Moustaid-Moussa and Carolyn D. Berdanier, CRC Press. 2001.
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