丙型肝炎病毒3a基因型初治和经治患者中NS5B对索磷布韦耐药性的鉴定。

Identification of NS5B resistance against SOFOSBUVIR in hepatitis C virus genotype 3a, naive and treated patients.

作者信息

Younas Saima, Sumrin Aleena, Hussain Nazim, Bilal Muhammad

机构信息

Centre for Applied Molecular Biology (CAMB), University of the Punjab, Lahore, Pakistan.

School of Life Science and Food Engineering, Huaiyin Institute of Technology, Huaian, China.

出版信息

J Appl Microbiol. 2022 Nov;133(5):2826-2834. doi: 10.1111/jam.15754. Epub 2022 Aug 11.

DOI:10.1111/jam.15754

PMID:35916643

Abstract

AIMS

Pakistan has the second highest prevalence of HCV with genotype 3a (GT-3a) being the most frequently circulating genotype. Currently, resistance-associated substitutions (RASs) are a major challenge in HCV treatment with direct-acting antivirals (DAAs). Sofosbuvir (SOF) is an FDA-approved NS5B nucleotide inhibitor. The aim of this study was to identify these RASs in the NS5B gene in naive and treated Pakistani HCV 3a isolates against SOF.

METHODS AND RESULTS

Blood samples were collected from anti-HCV-positive patients, followed by HCV RNA isolation and real-time PCR quantification. HCV-positive patients were processed for HCV RNA genotyping, patients with genotype 3a were processed for NS5B gene amplification and sequencing. GT-3a was the most prevalent genotype (62.2%). S282T was identified in 2 (8.7%) patients, C316Y/G/R in 3 (13%), V321A and L320P in 1 (4.3%) each in SOF/RBV-resistant patients. Variants of S282 were detected in 3 (13%) of SOF/RBV-treated patients. While INF/RBV-associated mutations were also analysed, D244N, A333R and A334E were identified in 2 (9.5%), 3 (14.2%) and 7 (33.3%) in treatment-naive and 15 (65.2%), 7 (30.4%) and 5 (21.7%) treated patients, respectively. Q309R was observed only in one treatment-experienced patients. Some substitutions were present at higher frequency in both groups like N307G, K304R, A272D and R345H, considered that they do not have any role in sofosbuvir resistance.

CONCLUSION

It was concluded that sofosbuvir RASs are present in Pakistani HCV GT-3a isolates, and they should be monitored carefully, especially in treatment-experienced patients, for further selection of treatment regimens.

SIGNIFICANCE AND IMPACT OF STUDY

HCV RASs have been studied very well across the world but there is scarcity of data regarding this topic in Pakistani population, this study provides data regarding the prevalence of these RASs in Pakistani HCV isolates emphasizing the fact that these RASs must be carefully monitored before starting HCV treatment, especially in treatment failure patients.

摘要

目的

巴基斯坦丙型肝炎病毒（HCV）感染率位居世界第二，其中基因3a型（GT-3a）是最常见的流行基因型。目前，耐药相关替代突变（RASs）是使用直接抗病毒药物（DAA）治疗HCV的主要挑战。索磷布韦（SOF）是一种经美国食品药品监督管理局（FDA）批准的NS5B核苷酸抑制剂。本研究的目的是在未经治疗和已接受治疗的巴基斯坦HCV 3a分离株的NS5B基因中鉴定这些RASs。

方法与结果

采集抗HCV阳性患者的血液样本，随后进行HCV RNA分离和实时PCR定量分析。对HCV阳性患者进行HCV RNA基因分型，对基因3a型患者进行NS5B基因扩增和测序。GT-3a是最常见的基因型（62.2%）。在接受SOF/利巴韦林（RBV）治疗耐药的患者中，2例（8.7%）检测到S282T，3例（13%）检测到C316Y/G/R，各有1例（4.3%）检测到V321A和L320P。在接受SOF/RBV治疗的患者中，3例（13%）检测到S282变异。同时分析了与干扰素/利巴韦林相关的突变，在未经治疗的患者中，2例（9.5%）、3例（14.2%）和7例（33.3%）分别检测到D244N、A333R和A334E，在接受治疗的患者中，分别有15例（65.2%）、7例（30.4%）和5例（21.7%）检测到这些突变。仅在1例有治疗史的患者中观察到Q309R。两组中一些替代突变的出现频率较高，如N307G、K304R、A272D和R345H，认为它们对索磷布韦耐药无作用。