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Host genetic factors associated with hepatocellular carcinoma in patients with hepatitis C virus infection: a systematic review

机译:丙型肝炎病毒感染患者与肝细胞癌相关的宿主遗传因素:系统评价

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摘要

Hepatitis C virus (HCV)-infected patients are at risk of developing hepatocellular carcinoma (HCC). Individuals at heightened riskcould be targeted by intensive follow-up surveillance. We have conducted a systematic review of the literature to identify host genetic predisposition to HCC in HCV-infected patients.\udA comprehensive search of Medline and Embase databases was performed and the strength of evidence of associations for each gene on development of HCC was evaluated.\udWe identified 166 relevant studies, relating to 137 different genes, or combinations thereof. 17 genes were classified as having “good” evidence of an association, a significant association was observed for 37 genes but this finding had not yet been replicated, 56 genes had mixed or limited evidence of an association, and 27 genes showed no association. IFNL3/4, TNF-α and PNPLA3 genes had the most evidence of an association. There was, however, considerable heterogeneity in study design and data quality.\udIn conclusion, we identified a number of genes with evidence of association with HCC, but also a need for more standardised approaches to address this clinically critical question. It is important to consider the underlying mechanism of these relationships and which are confounded by the presence of other HCC risk factors and response to therapy. We also identified many genes where the evidence of association is contradictory or requires replication, as well as a number where associations have been studied but no evidence found. These findings should help to direct future studies on host genetic predisposition to HCC in patients with HCV infection.
机译:感染丙型肝炎病毒(HCV)的患者有发展为肝细胞癌(HCC)的风险。可以通过加强的后续监视来确定高危人群的目标。我们对文献进行了系统的综述,以确定在HCV感染患者中HCC的宿主遗传易感性。\ ud对Medline和Embase数据库进行了全面搜索,并评估了每个基因与HCC发生关联的证据强度。 \ ud我们鉴定了166个相关研究,涉及137个不同基因或其组合。有17个基因被归类为具有“良好”关联证据,观察到37个基因有显着关联,但这一发现尚未被复制,有56个基因混合或关联证据有限,而27个基因则没有关联。 IFNL3 / 4,TNF-α和PNPLA3基因具有最大的关联性证据。但是,研究设计和数据质量存在相当大的异质性。\ ud最后,我们确定了许多与肝癌相关的基因,但也需要采用更加标准化的方法来解决这一临床关键问题。重要的是要考虑这些关系的潜在机制,并与其他HCC危险因素的存在和对治疗的反应相混淆。我们还鉴定了许多关联证据相互矛盾或需要复制的基因,以及一些已研究关联但未发现证据的基因。这些发现应有助于指导未来关于HCV感染患者肝癌宿主遗传易感性的研究。

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