Virological Departement Laboratoire Alphabio, Hôpital Ambroise Paré, Marseille, France.
J Hepatol. 2011 Jul;55(1):192-206. doi: 10.1016/j.jhep.2011.01.011. Epub 2011 Feb 1.
Recent advances in molecular biology have led to the development of novel small molecules that target specific viral proteins of the hepatitis C virus (HCV) life cycle. These drugs, collectively termed directly acting antivirals (DAA) against HCV, include a range of non-structural (NS) 3/NS4A protease, NS5B polymerase, and NS5A inhibitors at various stages of clinical development. The rapid replication rate of HCV, along with the low fidelity of its polymerase, gives rise to generations of mutations throughout the viral genome resulting in remarkable sequence variation in the HCV population, known as a quasispecies. The efficacy of DAAs is limited by the presence of those mutations that give rise to amino-acid substitutions within the targeted protein, and that affect the viral sensitivity to these compounds. Thus, due to the high genetic variability of HCV, variants with reduced susceptibility to DAA can occur naturally even before treatment begins, but usually at low levels. Not surprisingly then, these changes are selected in patients either breaking through or not responding to potent DAA treatment. In vitro or in vivo, six major position mutations in the NS3 HCV protease (36, 54, 155, 156, 168, and 170) have now been reported associated with different levels of resistance. The amino acid composition at several of the drug resistance sites can vary between the HCV genotypes/subtypes, resulting in different consensus amino acids leading to a reduction in replicative fitness as well as reduced DAA sensitivity. Different amino acid diversity profiles for HCV genotypes/subtypes suggest differences in the position/type of immune escape and drug resistance mutations. Also, different pathways of resistance profiles based on the chemical scaffold (linear or macrocyclic) of the protease inhibitors have been described. This review first describes how resistance to a protease inhibitor can develop and then provides an overview of the mechanism of how particular mutations confer varying levels of resistance to protease inhibitor, which have been identified and characterized using both genotypic and phenotypic tools. Future potential therapeutic strategies to assist patients who do develop resistance to protease inhibitors are also outlined. The challenge developing new HCV protease inhibitors should take into consideration not only the antiviral potency of the drugs, the occurrence and importance of side effects, the frequency of oral administration, but also the resistance profiles of these agents.
近年来,分子生物学的进展促使人们开发出了针对丙型肝炎病毒(HCV)生命周期中特定病毒蛋白的新型小分子药物。这些药物统称为直接作用抗病毒药物(DAA),包括一系列非结构(NS)3/NS4A 蛋白酶、NS5B 聚合酶和 NS5A 抑制剂,它们处于不同的临床开发阶段。HCV 的快速复制率以及其聚合酶的低保真度导致病毒基因组中产生大量突变,从而导致 HCV 群体中出现显著的序列变异,称为准种。DAA 的疗效受到那些导致靶向蛋白中氨基酸取代以及影响这些化合物对病毒敏感性的突变的限制。因此,由于 HCV 的高度遗传变异性,即使在开始治疗之前,对 DAA 敏感性降低的变体也可能自然存在,但通常水平较低。毫不奇怪,这些变化会在患者中选择,要么突破,要么对有效的 DAA 治疗没有反应。在体外或体内,现已报道 HCV 蛋白酶(36、54、155、156、168 和 170 位)中的 6 个主要位置突变与不同水平的耐药性有关。几个耐药性位点的氨基酸组成在 HCV 基因型/亚型之间有所不同,导致不同的共识氨基酸,从而降低复制适应性以及降低 DAA 敏感性。HCV 基因型/亚型的不同氨基酸多样性谱表明免疫逃避和耐药性突变的位置/类型存在差异。此外,还描述了基于蛋白酶抑制剂的化学支架(线性或大环)的不同耐药谱途径。这篇综述首先描述了对蛋白酶抑制剂的耐药性如何发展,然后概述了特定突变如何赋予对蛋白酶抑制剂的不同水平耐药性的机制,这些突变已使用基因型和表型工具进行了鉴定和特征描述。还概述了未来用于辅助对蛋白酶抑制剂产生耐药性的患者的潜在治疗策略。开发新的 HCV 蛋白酶抑制剂的挑战不仅应考虑药物的抗病毒效力、副作用的发生和重要性、口服给药的频率,还应考虑这些药物的耐药谱。
