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Association between the TIMD4-HAVCR1 variants and serum lipid levels coronary heart disease and ischemic stroke risk and atorvastatin lipid-lowering efficacy

机译:TIMD4-HAVCR1变异体与血脂水平冠心病缺血性中风风险和阿托伐他汀降脂功效之间的关联

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摘要

Little is known about the association of the TIMD4 (T-cell immunoglobulin and mucin domain 4 gene)-HAVCR1 (hepatitis A virus cellular receptor 1) variants and lipid metabolism, the risk of coronary heart disease (CHD) and ischemic stroke (IS). The present study aimed to determine the TIMD4-HAVCR1 variants, their haplotypes and gene–environment interactions on serum lipid levels, the risk of CHD and IS, and the lipid-lowering efficacy of atorvastatin in a southern Chinese Han population. Genotypes of three variants in 622 controls, 579 CHD, and 546 IS patients were determined by the Snapshot technology. Atorvastatin calcium tablet (20 mg/day) was given in 724 hyperlipidemic patients for 8 weeks after genotyping. The rs12522248 genotypic and allelic frequencies were different between controls and patients, and were associated with the risk of CHD and IS. The rs1501908G-rs12522248T-rs2036402T haplotype was associated with an increased risk of CHD; the G-C-T haplotype was associated with lower risk of CHD; and the C-C-C haplotype was associated with an increased risk of IS. Variants and their haplotypes in controls were associated with triglyceride (rs1501908), low-density lipoprotein cholesterol (LDL-C, rs1501908, G-T-T), high-density lipoprotein cholesterol (HDL-C, rs12522248, C-C-C) and the ratio of total cholesterol (TC) to HDL-C (C-C-C). Interactions of rs1501908- and rs2036402-alcohol (HDL-C); rs1501908- and rs12522248-high body mass index (hBMI, ≥24 kg/m2; TC); and TIMD4-HAVCR1 variants-atorvastatin on several lipid parameters were detected. Interactions of rs12522248TC/CC-hBMI, G-T-T-, and C-C-C-smoking on the risk of CHD; and C-C-C-smoking, C-C-C-, and G-C-T-hBMI on the risk of IS were also observed. These findings suggest that the TIMD4-HAVCR1 variants may be the genetic risk factors for CHD and IS.
机译:关于TIMD4(T细胞免疫球蛋白和粘蛋白结构域4基因)-HAVCR1(甲型肝炎病毒细胞受体1)变体与脂类代谢,冠心病(CHD)和缺血性中风(IS)的关联知之甚少。本研究旨在确定中国南部汉族人群中TIMD4-HAVCR1变异体,它们的单倍型和基因-环境相互作用对血脂水平,CHD和IS的风险以及阿托伐他汀的降脂功效。通过Snapshot技术确定了622名对照,579名CHD和546名IS患者的三种变异的基因型。基因分型后8周,对724名高脂血症患者给予阿托伐他汀钙片(20 mg /天)。 rs12522248的基因型和等位基因频率在对照组和患者之间是不同的,并且与CHD和IS的风险有关。 rs1501908G-rs12522248T-rs2036402T单倍型与冠心病风险增加相关; G-C-T单倍型与冠心病风险降低有关; C-C-C单倍型与IS风险增加有关。对照中的变体及其单倍型与甘油三酸酯(rs1501908),低密度脂蛋白胆固醇(LDL-C,rs1501908,GTT),高密度脂蛋白胆固醇(HDL-C,rs12522248,CCC)和总胆固醇比率( TC)转换为HDL-C(CCC)。 rs1501908-和rs2036402-酒精(HDL-C)的相互作用; rs1501908-和rs12522248-高体重指数(hBMI,≥24kg / m 2 ; TC);检测了一些脂质参数上的TIMD4-HAVCR1变体-阿托伐他汀。 rs12522248TC / CC-hBMI,G-T-T-和C-C-C吸烟与CHD风险的相互作用;还观察到吸烟,C-C-C-和G-C-T-hBMI对IS风险的影响。这些发现表明TIMD4-HAVCR1变异可能是CHD和IS的遗传危险因素。

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