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Recognition of genetic factors influencing the progression of hepatitis C : potential for personalized therapy.

机译:认识到影响丙型肝炎进展的遗传因素:个性化治疗的潜力。

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摘要

Infection with hepatitis C virus (HCV) is a major cause of chronic liver disease. Hepatic fibrosis may develop in subjects with chronic HCV infection, culminating in cirrhosis and an increased risk of hepatocellular carcinoma. The rate of development of fibrosis varies substantially between individuals; while it is influenced by a number of demographic and environmental factors, these account for only a small proportion of the variability.There are no clinical markers or tests that predict the rate of fibrosis progression in an individual subject. Thus, there has been increasing interest in the influence of host genetic factors on the rate of disease progression, and whether a genetic signature can be developed to reliably identify individuals at risk of severe disease. Numerous case-control, candidate gene, allele-association studies have examined the relationship between host single nucleotide polymorphisms or other genetic mutations and fibrosis in patients with chronic HCV infection. However, thesestudies have generally been irreproducible and disappointing. As seen with genetic studies for other diseases, small study cohorts and poor study design have contributed to limited meaningful findings. The successful determination of genetic signatures for fibrosis progression in chronic HCV will require multicenter collaborations using genome-wide association studies, with large, phenotypically well-defined sample sets. While these studies will require a significant financial commitment, a successful outcome offers the potential for personalized therapy and better patient management.
机译:丙型肝炎病毒(HCV)感染是慢性肝病的主要原因。患有慢性HCV感染的受试者可能会发生肝纤维化,最终导致肝硬化和肝细胞癌风险增加。个体之间纤维化的发生率差异很大。尽管受多种人口统计学和环境因素的影响,但这些因素仅占变异性的一小部分。尚无临床指标或测试可预测个体受试者纤维化进展的速度。因此,人们越来越关注宿主遗传因素对疾病进展速度的影响,以及是否可以开发遗传标记来可靠地识别处于严重疾病风险中的个体。大量病例对照,候选基因,等位基因关联研究已经研究了慢性HCV感染患者宿主单核苷酸多态性或其他基因突变与纤维化之间的关系。然而,这些研究通常是不可再现的并且令人失望。从对其他疾病的基因研究可以看出,较小的研究队列和不良的研究设计导致有限的有意义的发现。要成功确定慢性HCV纤维化进展的遗传特征,就需要使用全基因组关联研究与大型,表型明确的样本集进行多中心合作。尽管这些研究需要大量的财务投入,但成功的结果为个性化治疗和更好的患者管理提供了潜力。

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