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Rare Pathogenic Variants Predispose to Hepatocellular Carcinoma in Nonalcoholic Fatty Liver Disease

机译:罕见病原体易患非酒精性脂肪肝病的肝细胞癌

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摘要

Nonalcoholic fatty liver disease (NAFLD) is a rising cause of hepatocellular carcinoma (HCC). We examined whether inherited pathogenic variants in candidate genes (n = 181) were enriched in patients with NAFLD-HCC. To this end, we resequenced peripheral blood DNA of 142 NAFLD-HCC, 59 NAFLD with advanced fibrosis, and 50 controls, and considered 404 healthy individuals from 1000 G. Pathogenic variants were defined according to ClinVar, likely pathogenic as rare variants predicted to alter protein activity. In NAFLD-HCC patients, we detected an enrichment in pathogenic (p = 0.024), and likely pathogenic variants (p = 1.9*10−6), particularly in APOB (p = 0.047). APOB variants were associated with lower circulating triglycerides and higher HDL cholesterol (p < 0.01). A genetic risk score predicted NAFLD-HCC (OR 4.96, 3.29–7.55; p = 5.1*10−16), outperforming the diagnostic accuracy of common genetic risk variants, and of clinical risk factors (p < 0.05). In conclusion, rare pathogenic variants in genes involved in liver disease and cancer predisposition are associated with NAFLD-HCC development.
机译:非酒精性脂肪肝疾病(NAFLD)是肝细胞癌(HCC)的上升原因。我们检查了NAFLD-HCC患者中候选基因(n = 181)中遗传的致病变异是否丰富。为此,我们对142例NAFLD-HCC,59例晚期纤维化的NAFLD和50例对照的外周血DNA进行了重测序,并考虑了来自1000 G的404名健康个体。根据ClinVar定义了致病性变体,可能是致病性,是预计会改变的罕见变体蛋白质活性。在NAFLD-HCC患者中,我们检测到致病性(p = 0.024)和可能的致病变异(p = 1.9 * 10 -6 ),尤其是APOB(p = 0.047)富集。 APOB变异与较低的循环甘油三酸酯和较高的HDL胆固醇相关(p <0.01)。遗传风险评分可预测NAFLD-HCC(OR 4.96,3.29–7.55; p = 5.1 * 10 −16 ),胜过常见遗传风险变量和临床风险因素的诊断准确性(p < 0.05)。总之,与肝脏疾病和癌症易感性有关的基因中罕见的致病变异与NAFLD-HCC的发生有关。

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