Investigation of the MGP promoter and exon 4 polymorphisms in patients with ischemic stroke in the Ukrainian population

dc.contributor.authorОбухова, Ольга Анатоліївна
dc.contributor.authorОбухова, Ольга Анатольевна
dc.contributor.authorObukhova, Olha Anatoliivna
dc.contributor.authorГарбузова, Вікторія Юріївна
dc.contributor.authorГарбузова, Виктория Юрьевна
dc.contributor.authorHarbuzova, Viktoriia Yuriivna
dc.contributor.authorАтаман, Олександр Васильович
dc.contributor.authorАтаман, Александр Васильевич
dc.contributor.authorAtaman, Oleksandr Vasylovych
dc.contributor.authorАтаман, Юрій Олександрович
dc.contributor.authorАтаман, Юрий Александрович
dc.contributor.authorAtaman, Yurii Oleksandrovych
dc.contributor.authorMatlaj, O.I.
dc.date.accessioned2014-11-17T08:58:56Z
dc.date.available2014-11-17T08:58:56Z
dc.date.issued2012
dc.description.abstractMatrix γ-carboxyglutamic acid protein (MGP) is a vitamin K-dependent protein playing a pivotal role in preventing arterial calcification. In the present study, we aimed to investigate the relation between three single nucleotide polymorphisms of MGP gene and ischemic stroke (IS) in the Ukrainian population. 170 IS patients and 124 healthy controls were recruited to the study. MGP SNPs were examined by PCR-RFLP methodology. The distribution of homozygous carriers of the major allelic variant, and heterozygous and homozygous minor allele variants of the T-138C MGP promoter polymorphism (rs1800802) in patients with IS was 61.2%, 31.2% and 7.6%, respectively. The corresponding distributions of the variants in the control group were 59.7%, 35.6%, 4.8%. With regard to the G-7A promoter polymorphism (rs1800801), the respective distributions were 35.9%, 48.8% and 15.3%, compared to 43.5%, 50% and 6.5% in the control group. Finally, the respective distributions according to the Thr83Ala exon 4 polymorphism (rs4236) were 39.4%, 48.8% and 11.8%, compared to 34.7%, 53.2% and 12.1% in the control group. Using logistic regression analysis, it was estimated that A/A genotype (G-7A polymorphism) was significantly (P=0.016) associated with IS (OR=2.943; 95% CI: 1.218–7.109) in the Ukrainian population. A-allele homozygotes of female sex had a risk of IS more than 7 times higher compared with carriers of G/G genotype.ru_RU
dc.identifier.citationInvestigation of the MGP promoter and exon 4 polymorphisms in patients with ischemic stroke in the Ukrainian population [Текст] / A.V. Ataman, V.Yu. Garbuzova, Yu.A. Ataman et al. // Journal of Cell and Molecular Biology. – 2012. – Vol.10, №1. – С. 19-26.ru_RU
dc.identifier.sici0000-0002-1941-740Xen
dc.identifier.urihttp://essuir.sumdu.edu.ua/handle/123456789/37742
dc.language.isoenru_RU
dc.publisherHaliç University, Printed in Turkeyru_RU
dc.rights.uricneen_US
dc.subjectматриксний Gla-протеїнru_RU
dc.subjectматриксный Gla-протеинru_RU
dc.subjectMatrix Gla proteinru_RU
dc.subjectполіморфізмru_RU
dc.subjectполиморфизмru_RU
dc.subjectsingle nucleotide polymorphismru_RU
dc.subjectішемічний інсультru_RU
dc.subjectишемический инсультru_RU
dc.subjectischemic strokeru_RU
dc.subjectкальцифікація судинru_RU
dc.subjectкальцификация сосудовru_RU
dc.subjectarterial calcificationru_RU
dc.subjectукраїнська популяціяru_RU
dc.subjectукраинская популяцияru_RU
dc.subjectukrainian populationru_RU
dc.titleInvestigation of the MGP promoter and exon 4 polymorphisms in patients with ischemic stroke in the Ukrainian populationru_RU
dc.typeArticleru_RU

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