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effect of mthfr a1298c gene polymorphism on acute coronary syndrome
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نویسنده
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fuadi muhamad robiul ,nugraha jusak r. ,suryawan i gde rurus ,kahar hartono ,aryati aryati ,prabowo gwenny ichsan ,utomo budi ,i'tishom reny
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منبع
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arya atherosclerosis - 2023 - دوره : 19 - شماره : 2 - صفحه:77 -82
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چکیده
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Background: cardiovascular disease (cvd) is the leading cause of mortality worldwide. acute coronary syndrome is a manifestation of cvd. in indonesia, limited studies have been conducted on genetics as a potential risk factor for acute coronary syndrome (acs). consequently, this study aimed to examine the effect of the methylenetetrahydrofolate reductase (mthfr) a1298c gene polymorphism on the incidence of acs.methods: the study employed a case-control design. outpatients from the cardiology and internal medicine clinics at the university of airlangga (unair) hospital in surabaya, indonesia, constituted the study population. the case group comprised 60 patients with a history of acs, while the control group consisted of 30 patients without a history of cardiovascular complaints. mthfr a12980c gene polymorphism examination was performed using the polymerase chain reaction-restriction fragment length polymorphism (pcr rflp) method at the tropical disease center unair laboratory.results: among the acs group, 29 (48.1%), 13 (21.7%), and 18 (30%) of the individuals had aa, ac, and cc genotype patterns, respectively. in the control group, 16 individuals had aa (53.3%), 6 ac (20%), and 8 cc (26.7%). the c allele variant was identified in 41% of the acs group and 37% of the control group. the odds ratio (or) for the incidence of acs was 1.195 (95% confidence interval [ci]; 0.381-3.752), 1.241 (95% ci; 0.481-3.486), and 1.222 (95% ci; 0.381-3.752). chi-square analysis revealed no association between mthfr a1298c gene polymorphism and the incidence of acs (p > 0.05).conclusions: mthfr a1298c gene polymorphism did not significantly affect acs incidence.
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کلیدواژه
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cardiovascular disease ,risk factors ,genetic ,polymerase chain reaction ,restriction fragment length polymorphism
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آدرس
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universitas airlangga, faculty of medicine, doctoral program of medical science, indonesia, universitas airlangga, faculty of medicine, department of clinical pathology, indonesia, universitas airlangga, faculty of medicine, department of cardiology and vascular medicine, iran, universitas airlangga, faculty of medicine, department of clinical pathology, indonesia, universitas airlangga, faculty of medicine, department of clinical pathology, indonesia, universitas airlangga, faculty of medicine, department of physiology and medical biochemistry, indonesia, universitas airlangga, faculty of medicine, department of public health and preventive medicine, indonesia, universitas airlangga, faculty of medicine, department of medical biology, indonesia
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پست الکترونیکی
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ritishom@fk.unair.ac.id
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Authors
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