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Understanding pathogenesis of
endometriosis and new
treatment modalities
Erkut Attar, M.D. PhD.
Istanbul University
Istanbul Medical School
Department of Obstetrics & Gynecology
Division of Reproductive Endocrinology & Infertility
In memory of Professor Oktay Kadayıfcı
The Golden Rule: Treat others how you want to be treated...
2
Endometriosis?
■
Affects nearly 1 in 7 women of reproductive age
■ Third most common gynecologic disorder that requires
hospitalization, and a leading cause of hysterectomy
■ Literature and other available data suggest that
endometriosis places a considerable burden on
patients and society
■
No new treatment modalities
since the last two decades
Current areas of research in the
etiopathogenesis of endometriosis
■
■
■
■
■
■
Immunology
Environmental Science
Genetics
Cancer Biology
Hormonal factors
Steroidogenesis
Attar E Endometriosis. In: The Endometrium, Ed. Fazlebas A. 2nd Edition,
Taylor Francis Books Ltd
Normal Endometrium and Endometriosis
5
ENDOMETRIUM
(NORMAL)
ENDOMETRIUM
(ENDOMETRIOSIS)
ENDOMETRIOTIC
TISSUE
COUP-TF
COUP-TF
WT-1
COX2
PGE2
COUP-TF
WT-1
SF-1
StAR?
Aromatase
COX2
E2
PGE2
WT-1
SF-1
StAR
Aromatase
COX2
E2
PGE2
Attar E and S.E. Bulun, Hum Reprod Update.2005; 0: 341
Epithelial Cell
Arachidonic Acid
IL1-
COX-2
VEGF
INFLAMMATION
Cholesterol
PGE2
cAMP
E2
GROWTH
StAR
Aromatase
Adrenal
Ovary
E1
A
Endometriotic Cell
Attar E and S.E. Bulun, Hum Reprod Update.2005; 0: 341
Molecular distinction between endometrium and endometriotic tissue
8
Disrupted paracrine action of progesterone
11
Epigenethic Changes in Endometriosis
12
Speculated Changes in DNA Methylation from Genetic or E
13
New Drugs?
■
Local aromatase gene expression and enzyme
activity were demonstrated in endometriotic
implants
■ Recently, we showed that aromatase enzyme
inhibitors treat endometriosis successfully
■ However, current aromatase inhibitors cause
total body estrogen deprivation regardless of
promoter use
PII regulates aromatase synthesis in endometriotic cells
AA
COX-2
PGE2
PGH2
cAMP
Co-Act (1)
C/EBP
Enh
CRS
Placenta
AROMATASE
Co-Act (2)
SF-1
X
PII II
NRHS
Skin/
Adipose
Brain
Bone
Adipose/
Cancer
Ovary/
Endometriosis
ATG
I.2a
5´
Coding region
I.4
I.1
I.7
I.f
I.6
I.3
PII
II
3´
X
AG/GACT
COMMON
SPLICE
SITE
TELOMERE
CYP19
CENTROMERE
What is NaBu?
■
■
■
■
■
■
A natural compound
A four carbon fatty acid
Inhibits histone deacetylase activity
inhibits growth arrest and induces cell
differentiation
induces apoptosis in vitro in cancer cells
MECHANISM of anti-neoplastic activity?
Why it is important to test this compound
in endometriosis?
■
■
■
■
orally administered
clinically evaluated in a phase I study
for a solid tumor
inhibits aromatase expression
A NEW DRUG for the treatment
endometriosis?
Endometriotic Cells 24h Treatment
0.5
0.4
PMol/mg
0.3
*p<0.01
*
0.2
**p<0.01
**
0.1
0.0
Control
5 mM/mL
10 mM/mL
15 mM/mL
The effect of NaBu on JEG-3 Cells
(Choriocarcinoma cell line)
18
*P<0.05
16
**P<0.05
**
*
14
pmol/mg
12
10
8
6
4
2
0
C
NaBu
cAMP
cAMP+NaBU
NaBu inhibits ATF-2 binding to
Promoter II
NaBu (mM/mL)
0
5
10
15
A
B
C
A: ATF-2
B: IgG
C:Input
Summary
PGE2
or
cAMP
PKA
p38
TauT
PKC
JNK
SB202190
AS601245
P
ATF-2
P
c-jun
Promoter II
Animal Models of Endometriosis
NaBu use in an animal model
Conclusion
■
Nutrition: Treatment and
Prevention?
■
■
■
■
■
Vitamin D, RA and...
Food intake
Prevention during pregnancy?
Histone deacetylase inhibitors
(NaBU)
More...
25
Thank You…
Northwestern Group
Serdar. Bulun, MD. (PI)
Dong Chen, PhD.
Santanu Deb.,PhD.
Masahi Demura, MD.
Veysel Fenkci,MD.
Gonca Imir,MD.
Scott Reieresterad
Hiroki Utsinomia, MD.
Bertan Yılmaz,PhD.
Ping Yin, PhD.
Istanbul Group
Rukset Attar, MD., PhD.
Narter Yeşildağlar, MD.
Pelin Balcık, MS