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Dynamic noninvasive markers predict hepatocellular carcinoma in chronic hepatitis C patients without sustained virological response after interferon-based therapy: Prioritize who needs urgent direct-acting antiviral agents

机译:动态无创标记物可预测慢性丙型肝炎患者在以干扰素为基础的治疗后无持续病毒学应答的肝细胞癌:确定谁需要紧急的直接作用抗病毒药物

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Some patients with hepatitis C virus (HCV) infections who fail to achieve sustained virological responses (SVRs) after interferon (IFN) therapy do not develop hepatocellular carcinoma (HCC). Risk stratification of these patients may help identify those who would benefit most from treatment with direct-acting antivirals (DAAs). A total of 552 HCV-infected patients with non-SVR status were enrolled. Laboratory data before and after IFN treatment were analyzed to determine the relationship of changes in serum markers with development of HCC during the 7-year study period. HCC developed in 93 patients. The risk factors for HCC were pre-existing liver cirrhosis, low hemoglobin level at baseline, low pretreatment platelet count, high post-treatment alpha-fetoprotein (AFP) level (≥15 ng/mL), and high post-treatment Fibrosis 4 (FIB4) index (>3.25). For patients without pre-existing cirrhosis, those with high post-treatment AFP level and FIB4 index had the highest risk of HCC (1 year: 6.7%; 3 years: 10.9%; 5 years: 29.7%), followed by those with high post-treatment AFP level and low post-treatment FIB4 index (5 years: 25%), and those with low post-treatment AFP level and high post-treatment FIB4 index (1 year: 3.7%; 3 years: 5.2%; 5 years: 10.6%). The risk was even lower for patients with low post-treatment AFP level and FIB4 index (1 year: 0%; 3 years: 0.4%; 5 years: 2.5%). None of the patients with FIB4 indexes consistently below 1.45 developed HCC. The combined use of post-treatment AFP level and FIB4 index was useful for risk stratification of HCV-infected patients with non-SVR status after IFN therapy. These data may help clinicians to identify patients who most urgently need DAA treatment.
机译:一些患有丙型肝炎病毒(HCV)感染的患者在干扰素(IFN)治疗后未能实现持续的病毒学应答(SVR),不会发展为肝细胞癌(HCC)。这些患者的风险分层可能有助于确定哪些患者将从直接作用抗病毒药(DAA)的治疗中受益最大。共有552名非SVR状态的HCV感染患者入组。分析了IFN治疗前后的实验室数据,以确定7年研究期间血清标志物变化与HCC发生的关系。 93例患者发生了HCC。肝癌的危险因素是既往肝硬化,基线血红蛋白水平低,治疗前血小板计数低,治疗后甲胎蛋白(AFP)水平高(≥15ng / mL)和治疗后纤维化4( FIB4)索引(> 3.25)。对于没有肝硬化的患者,治疗后AFP水平和FIB4指数高的患者发生肝癌的风险最高(1年:6.7%; 3年:10.9%; 5年:29.7%),其次是高肝癌的患者。治疗后AFP水平低且治疗后FIB4指数低(5年:25%),以及治疗后AFP水平低且治疗后FIB4指数高的患者(1年:3.7%; 3年:5.2%; 5年:10.6%)。对于治疗后AFP水平和FIB4指数较低的患者,风险甚至更低(1年:0%; 3年:0.4%; 5年:2.5%)。 FIB4指数始终低于1.45的患者均未出现HCC。治疗后AFP水平和FIB4指数的结合使用对于HCV感染,非SVR状态的HCV感染患者在IFN治疗后的风险分层很有用。这些数据可以帮助临床医生确定最需要DAA治疗的患者。

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