TITLE:
NOS3 894G > T Gene Polymorphism: A Potential Risk Factor of Stroke in Bahraini Patients
AUTHORS:
Manal A. Fadl, Adel A. AlJishi, Safa Taha, Moiz Bakhiet
KEYWORDS:
Gene Polymorphisms, Nitric Oxide Synthase, Stroke Risk Factors
JOURNAL NAME:
World Journal of Neuroscience,
Vol.8 No.1,
February
13,
2018
ABSTRACT: The endothelial nitric oxide synthase (eNOS) encoded by the NOS3 gene is responsible for the
synthesis of a vasoactive endothelium-derived nitric oxide (NO). The genetic
polymorphism of this gene explains, in part, why some people are prone to
develop stroke than others. In this study we conducted a case control study in
Bahrainis to investigate “for the first time” the relationship between NOS3 894G > T (rs1799983) and 786T > C (rs2070744) polymorphisms with the stroke predisposition in Bahraini
population. Detection of NOS3
polymorphism was performed by PCR RFLP genotyping method. The level of NO among
cases and controls was measured using ELISA. A total of 93 unrelated stroke
patients and 86 controls were included in the study. The three types of stroke;
Ischemic, hemorrhagic and transient ischemic attack were reported (91.4%, 7.5%
and 1.1% respectively). No significant gender difference was observed (P = 0.74). Having previous stroke was a
highly significant risk factor of the disease (P = 0.001, OR = 1.4), where as a family history of stroke was not
(OR = 0.11). The analysis provides evidence that the mutant 894GT + TT
genotypes of NOS3 894G > T polymorphism were positively associated with stroke predisposition and
it increased the risk of stroke nearly two folds (P = 0.037, OR = 1.936). Although we found an association between the mutant genotype786 TC + CC of
the NOS3 786T > C
polymorphism with the susceptibility to stroke (P = 0.023) suggesting that the mutant C allele might have a
protective effect against stroke in this population, the strength of this
association was rather low (OR = 0.484). The level of NO in stroke patients was
significantly low compared to healthy controls (P 0.005). Diabetes, hypertension, heart diseases were reported in stroke
patients (67%, 71.4% and 52.1% respectively). More
over 50% of the cases with previous stroke are both diabetic and hypertensive.
This indicates that these diseases could be considered as a significant factor
in the development of stroke in this population. We concluded that the NOS3-894 G > T
polymorphism is a potential risk factor of stroke in Bahraini population,
whereas as the NOS3 786T > C
polymorphism might have a possible protective role against the disease in this
population.