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首页> 外文期刊>Internal medicine. >Role of NS5A-L31/Y93 Double Wild-type in Failure of Glecaprevir/Pibrentasvir Double Therapy in Two Patients with a History of Direct-acting Antiviral Agent Failure: An Ultra-deep Sequencing Analysis
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Role of NS5A-L31/Y93 Double Wild-type in Failure of Glecaprevir/Pibrentasvir Double Therapy in Two Patients with a History of Direct-acting Antiviral Agent Failure: An Ultra-deep Sequencing Analysis

机译:NS5A-L31 / Y93双重野生型在两名有直接作用抗病毒药物失败史的患者中用Glecaprevir / Pibrentasvir双重治疗失败的作用:超深度测序分析

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摘要

We experienced two cases of hepatitis C virus (HCV) eradication failure in patients with a history of non-responsiveness to previous treatments with direct-acting antiviral agents (DAAs) who were subsequently treated with the combination of glecaprevir and pibrentasvir (GLE/PIB). Direct sequencing at commencement of GLE/PIB therapy showed non-structural protein (NS) 5A-P32 deletion in the first patient and NS5A-R30E/Q54H/A92K in the second patient (both genotype 1b). The common point was that L31/Y93 was double wild-type, and the IL28B polymorphism was non-TT type. Even when L31/Y93 is double wild-type, other NS5A mutations may affect the DAA re-treatment outcome. We analyzed the transition of amino acid mutations at NS5A by ultra-deep sequencing.
机译:我们曾有两例丙型肝炎病毒(HCV)根除失败的病史,这些患者对以前使用直接作用抗病毒药物(DAA)的治疗无反应的病史,随后接受格列卡韦和吡溴那韦(GLE / PIB)的联合治疗。 GLE / PIB治疗开始时的直接测序显示第一例患者的非结构蛋白(NS)5A-P32缺失,第二例患者的NS5A-R30E / Q54H / A92K(均为基因型1b)。共同点是L31 / Y93是双重野生型,而IL28B多态性是非TT型。即使当L31 / Y93是双重野生型时,其他NS5A突变也可能影响DAA的再治疗结果。我们通过超深度测序分析了NS5A氨基酸突变的转变。

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