The -863 TNF- Polymorphism and Primary Open Angle Glaucoma in Egyptians
• 2017
معلومات البحث
المؤلفون
1
Walaa Bayoumie El Gazzar,
1
Shaymaa Mohamed Abd El Rahman,
2
Mohamed Nagy Elmohamady,
2
Ahmed Mohamed Saeed and
2
Usama Shalaby
الكلمات المفتاحية
Polymorphism, PCR-RFLP, POAG, TNF-α, Glaucoma
المجلة العلمية
Not Available
الناشر
Not Available
المجلد
Not Available
العدد
Not Available
الصفحات
Not Available
publication.type
International
رابط البحث
Not Available
المواد المرفقة
Not Available
الملخص
Growing evidence indicates that TNF-alpha is involved in the
pathogenesis of POAG in several ways, primarly by induction of retinal
ganglion cells apoptosis and therefore optic nerve degeneration. TNF-alpha
and POAG relationship has been studied at the genetic level with variable
results in different populations. The transcription rate and the release of
the TNF-alpha cytokine have been reported to be affected by
polymorphisms in the promoter of the TNF- alpha gene. Polymorphisms at
positions -238 and -308 are the most frequent studied. Another
polymorphism, at the position -863 in the promoter region, has been less
studied, but a homozygous AA allele appears protective in a Chinese
population. Our aim was to assess the potential association of -863C/A
TNF-alpha gene promoter polymorphisms with POAG in an Egyptian
group of subjects. Genotyping of the TNF-alpha (-863) polymorphism
was done for 228 POAG patients and 230 control subjects using the PCRbased,
Restriction Fragment Length Polymorphism (RFLP) assay. TNFalpha
(-863) A/A genotype was absent in both groups. There was no
significant difference between both groups as regards to TNF-α (-863) A
allele carriage (6.14 versus 10.43%; p = 0. 099)). Also the genotype TNF-α
(-863) C/C and the frequency of the tumor necrosis factor-alpha (-863) C
allele did not significantly differ between both groups (93.86 versus 89.57%;
p = 0. 099) and 96.93 versus 94.78%; p = 0. 107) respectively. Our data
indicated that the TNF-alpha (-863) a allele is not linked with primary open
angle glaucoma protection among Egyptian patients.
pathogenesis of POAG in several ways, primarly by induction of retinal
ganglion cells apoptosis and therefore optic nerve degeneration. TNF-alpha
and POAG relationship has been studied at the genetic level with variable
results in different populations. The transcription rate and the release of
the TNF-alpha cytokine have been reported to be affected by
polymorphisms in the promoter of the TNF- alpha gene. Polymorphisms at
positions -238 and -308 are the most frequent studied. Another
polymorphism, at the position -863 in the promoter region, has been less
studied, but a homozygous AA allele appears protective in a Chinese
population. Our aim was to assess the potential association of -863C/A
TNF-alpha gene promoter polymorphisms with POAG in an Egyptian
group of subjects. Genotyping of the TNF-alpha (-863) polymorphism
was done for 228 POAG patients and 230 control subjects using the PCRbased,
Restriction Fragment Length Polymorphism (RFLP) assay. TNFalpha
(-863) A/A genotype was absent in both groups. There was no
significant difference between both groups as regards to TNF-α (-863) A
allele carriage (6.14 versus 10.43%; p = 0. 099)). Also the genotype TNF-α
(-863) C/C and the frequency of the tumor necrosis factor-alpha (-863) C
allele did not significantly differ between both groups (93.86 versus 89.57%;
p = 0. 099) and 96.93 versus 94.78%; p = 0. 107) respectively. Our data
indicated that the TNF-alpha (-863) a allele is not linked with primary open
angle glaucoma protection among Egyptian patients.
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