直接作用抗病毒药物达拉他韦和asunaprevir 治疗丙型肝炎病毒 1b 型患者的病毒学逃逸特征。
Characterization of virologic escape in hepatitis C virus genotype 1b patients treated with the direct-acting antivirals daclatasvir and asunaprevir.
机构信息
Sapporo Kosei General Hospital, Sapporo, Japan.
出版信息
J Hepatol. 2013 Apr;58(4):646-54. doi: 10.1016/j.jhep.2012.11.012. Epub 2012 Nov 22.
BACKGROUND & AIMS: Daclatasvir and asunaprevir are NS5A and NS3 protease-targeted antivirals currently under development for treatment of chronic hepatitis C virus infection. Clinical data on baseline and on-treatment correlates of drug resistance and response to these agents are currently limited.
METHODS
Hepatitis C virus genotype 1b Japanese patients (prior null responders to PegIFN-α/RBV [n=21] or PegIFN-α/RBV ineligible or intolerant [n=22]) were administered daclatasvir/asunaprevir for 24 weeks during a phase 2a open-label study. Genotypic and phenotypic analyses of NS3 and NS5A substitutions were performed at baseline, after virologic failure, and post-treatment through follow-up week 36.
RESULTS
There were three viral breakthroughs and four relapsers. Baseline NS3 polymorphisms (T54S, Q80L, V170M) at amino acid positions previously associated with low-level resistance (<9-fold) to select NS3 protease inhibitors were detected in four null responders and three ineligibles, but were not associated with virologic failure. Baseline NS5A polymorphisms (L28M, L31M, Y93H) associated with daclatasvir resistance (<25-fold) were detected in five null responders and six ineligibles. All three viral breakthroughs and 2/4 relapsers carried a baseline NS5A-Y93H polymorphism. NS3 and NS5A resistance-associated variants were detected together (NS3-D168A/V, NS5A-L31M/V-Y93H) after virologic failure. Generally, daclatasvir-resistant substitutions persisted through 48weeks post-treatment, whereas asunaprevir-resistant substitutions were no longer detectable. Overall, 5/10 patients with baseline NS5A-Y93H experienced virologic failure, while 5/10 achieved a sustained virologic response.
CONCLUSIONS
The potential association of a pre-existing NS5A-Y93H polymorphism with virologic failure on daclatasvir/asunaprevir combination treatment will be examined in larger studies. The persistence of treatment-emergent daclatasvir- and asunaprevir-resistant substitutions will require assessment in longer-term follow-up studies.
背景与目的
达卡他韦和asunaprevir 是目前正在开发的用于治疗慢性丙型肝炎病毒感染的 NS5A 和 NS3 蛋白酶靶向抗病毒药物。目前,关于这些药物耐药性和应答的基线和治疗中相关因素的临床数据有限。
方法
在一项 2a 期开放标签研究中,21 例既往聚乙二醇干扰素-α/利巴韦林(PegIFN-α/RBV)无应答或 PegIFN-α/RBV 不适用或不耐受的丙型肝炎病毒 1b 型日本患者(n=21)和 22 例不适用或不耐受 PegIFN-α/RBV 的患者接受了达卡他韦/asunaprevir 治疗 24 周。在病毒学失败后和治疗后随访第 36 周时,对 NS3 和 NS5A 替换的基因型和表型分析进行了基线检测。
结果
有 3 例病毒学突破和 4 例复发。在 4 例无应答者和 3 例不适用者中检测到了先前与低水平(<9 倍)对选择的 NS3 蛋白酶抑制剂耐药相关的 NS3 氨基酸位置(T54S、Q80L、V170M)多态性,但与病毒学失败无关。在 5 例无应答者和 6 例不适用者中检测到与达卡他韦耐药相关的 NS5A 多态性(L28M、L31M、Y93H)(<25 倍)。所有 3 例病毒学突破和 2/4 例复发均携带基线 NS5A-Y93H 多态性。在病毒学失败后检测到 NS3 和 NS5A 耐药相关变异体的共同存在(NS3-D168A/V、NS5A-L31M/V-Y93H)。一般来说,达卡他韦耐药性替换在治疗后 48 周时持续存在,而asunaprevir 耐药性替换不再可检测到。总的来说,10 例基线 NS5A-Y93H 患者中有 5 例发生病毒学失败,而 10 例获得持续病毒学应答。
结论
在更大的研究中,将进一步研究基线 NS5A-Y93H 多态性与达卡他韦/asunaprevir 联合治疗的病毒学失败之间的潜在关联。在更长时间的随访研究中,需要评估治疗后出现的达卡他韦和asunaprevir 耐药替换的持续性。
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