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首页> 外文期刊>American Journal of Epidemiology >A field synopsis and meta-analysis of genetic association studies in peripheral arterial disease: The CUMAGAS-PAD database.
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A field synopsis and meta-analysis of genetic association studies in peripheral arterial disease: The CUMAGAS-PAD database.

机译:外周动脉疾病遗传关联研究的现场简介和荟萃分析:CUMAGAS-PAD数据库。

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In an electronic search of the literature, the authors systematically retrieved all published studies that investigated genetic susceptibility to peripheral arterial disease (PAD). They created a comprehensive database of all eligible studies, collecting detailed genetic and bioinformatics data on each polymorphism. Data from eligible studies were synthesized using meta-analysis techniques. Gene variants were classified into distinct pathophysiologic pathways, and their potential involvement in PAD pathogenesis was determined. Forty-one publications that examined 44 gene polymorphisms were included. For 37 polymorphisms, the variant form had a functional effect. Twenty-three polymorphisms in 22 potential PAD candidate genes (F2, FGB, MTHFR, ITGB3, ACE, AGT, IL6, CCL2, ICAM1, SELE, MMP9, PPARG, MMP1, ADD1, P2RY12, LIPC, PLA2G7, SCARB1, MMP3, MTTP, LPA, CHRNA3) showed a significant association in individual studies. Eighty-eight percent of the studies had statistical power of less than 50%, and in 15 studies the genotype distribution in the control group did not conform to Hardy-Weinberg equilibrium. Data on 12 polymorphisms (F5 1691 G/A, MTHFR 677C/T, F2 20210 G/A, ITGB3 1565 T/C, ACE I/D, AGT 704C/T, AGT -6G/A, AGT 733C/T, IL6 -174 G/C, MMP9 -1562C/T, ICAM1 1462A/G, CHRNA3 831C/T) were synthesized, and a positive association was found for 3 (IL6 -174 G/C, ICAM1 1462A/G, CHRNA3 831C/T).
机译:在电子检索文献中,作者系统地检索了所有已发表的研究,这些研究调查了对外周动脉疾病(PAD)的遗传易感性。他们创建了一个包含所有合格研究的综合数据库,收集了有关每种多态性的详细遗传和生物信息学数据。使用荟萃分析技术对来自合格研究的数据进行了综合。基因变体被分为不同的病理生理途径,并确定了它们在PAD发病机理中的潜在作用。包括检查44种基因多态性的41个出版物。对于37个多态性,变体形式具有功能作用。 22个潜在的PAD候选基因(F2,FGB,MTHFR,ITGB3,ACE,AGT,IL6,CCL2,ICAM1,SELE,MMP9,PPARG,MMP1,ADD1,P2RY12,LIPC,PLA2G7,SCARB1,MMP3,MTTP ,LPA,CHRNA3)在个别研究中显示出显着的关联。 88%的研究的统计功效低于50%,在15个研究中,对照组的基因型分布不符合Hardy-Weinberg平衡。 12种多态性的数据(F5 1691 G / A,MTHFR 677C / T,F2 20210 G / A,ITGB3 1565 T / C,ACE I / D,AGT 704C / T,AGT -6G / A,AGT 733C / T,IL6合成了-174 G / C,MMP9 -1562C / T,ICAM1 1462A / G,CHRNA3 831C / T,发现3(IL6 -174 G / C,ICAM1 1462A / G,CHRNA3 831C / T正相关)。

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