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首页> 外文期刊>American journal of medical genetics, Part C. Seminars in medical genetics >Genetic variants in rheumatic fever and rheumatic heart disease
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Genetic variants in rheumatic fever and rheumatic heart disease

机译:风湿热和风湿性心脏病的遗传变异

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摘要

Genetic association studies in rheumatic heart disease (RHD) have the potential to contribute toward our understanding of the pathogenetic mechanism, and may shed light on controversies about RHD etiology. Furthermore, genetic association studies may uncover biomarkers that can be used to identify susceptible individuals, and contribute toward developing vaccine and novel therapeutic targets. Genetic predisposition to rheumatic fever and RHD has been hypothesized by findings from familial studies and observed associations between genes located in the human leukocyte antigens on chromosome 6p21.3 and elsewhere in the genome. We sought to summarize, from published Genetic association studies in RHD, evidence on genetic variants implicated in RHD susceptibility. Using HuGENet (TM) systematic review methods, we evaluated 66 studies reporting on 42 genes. Existing meta-analyses of candidate gene studies suggest that TGF-beta 1 [rs1800469], and IL-1 beta [rs2853550] single nucleotide polymorphisms (SNPs) contribute to susceptibility to RHD, whereas the TNF-alpha [rs1800629 and rs361525], TGF-beta 1 [rs1800470 and rs4803457], IL-6 [rs1800795], IL-10 [rs1800896] were not associated with RHD. However, candidate gene studies in RF/RHD are relatively small, thus lacking statistical power to identify reliable and reproducible findings, emphasizing the need for large-scale multicenter studies with different populations.
机译:遗传关联研究中的风湿病疾病(RHD)有可能有助于我们对致病机制的理解,并且可以在rhD病因的争议中阐明。此外,遗传结合研究可以揭示可用于鉴定易感个体的生物标志物,并有助于发育疫苗和新的治疗靶标。对风湿热和RHD的遗传倾向已经假设来自家族研究的结果和观察到位于染色体的人白细胞抗原的基因之间的基因之间的关联和基因组中的其他地方。我们试图从发表的RHD中发表的遗传关联研究总结,有关遗传变异的证据涉及RHD易感性。使用Hugenet(TM)系统评价方法,我们评估了66项关于42个基因的研究报告。候选基因研究的现有荟萃分析表明,TGF-β1[RS1800469]和IL-1β[RS2853550]单核苷酸多态性(SNPS)有助于rhD的易感性,而TNF-α[RS1800629和RS361525],TGF -beta 1 [RS1800470和RS4803457],IL-6 [RS1800795],IL-10 [RS1800896]与RHD无关。然而,RF / RHD中的候选基因研究相对较小,因此缺乏鉴定可靠和可重复的发现的统计能力,强调需要具有不同群体的大规模多中心研究。

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