全球86种丙型肝炎病毒亚型中基因 、 和 中天然存在的抗性相关替代的计算分析。
Computational analysis of naturally occurring resistance-associated substitutions in genes , , and among 86 subtypes of hepatitis C virus worldwide.
作者信息
Wu Ruihong, Geng Dongfeng, Chi Xiumei, Wang Xiaomei, Gao Xiuzhu, Xu Hongqin, Shi Ying, Guan Yazhe, Wang Yang, Jin Jinglan, Ding Yanhua, Niu Junqi
机构信息
Department of Hepatology, First Hospital of Jilin University, Changchun, Jilin Province 130021, People's Republic of China.
Centre for Reproductive Medicine, Centre for Prenatal Diagnosis, First Hospital of Jilin University, Changchun, Jilin Province 130021, People's Republic of China.
出版信息
Infect Drug Resist. 2019 Sep 19;12:2987-3015. doi: 10.2147/IDR.S218584. eCollection 2019.
BACKGROUND AND OBJECTIVE
Direct-acting antivirals (DAA) facing resistance continue to be used in some areas worldwide. Thus, identifying hepatitis C virus (HCV) genotypes/subtypes and loci with certain prevalent resistance-associated substitutions (RASs) deserves attention. We investigated the global and regional frequencies of naturally occurring RASs among all confirmed HCV subtypes (n=86) and explored co-occurring and mutually exclusive RAS pairs within and between genes , , and .
METHODS
A total of 213,908 HCV sequences available as of July 10, 2019 were retrieved from the NCBI nucleotide database. After curation, 17,312 NS3, 8,478 NS5A, and 25,991 NS5B sequence fragments from DAA-naïve patients were screened for RASs. MEGA 6.0 was used to translate aligned nucleotide sequences into amino acid sequences, and RAS pairs were identified by hypergeometric analysis.
RESULTS
RAS prevalence varied significantly among HCV subtypes. For example, D168E, highly resistanct to all protease inhibitors except voxilaprevir, was nearly absent in all subtypes except in 43.48% of GT5a sequences. RASs in NS3 exhibiting significantly different global distribution included Q80K in GT1a with the highest frequency in North America (54.49%), followed by in Europe (22.66%), Asia (6.98%), Oceania (6.62%), and South America (1.03%). The prevalence of NS3 S122G in GT1b was highest in Asia (26.6%) and lowest in Europe (2.64%). NS5A L28M, R30Q, and Y93H in GT1b, L31M in GT2b, and NS5B C316N in GT1b was most prevalent in Asia. A150V in GT3a, associated with sofosbuvir treatment failure, was most prevalent in Asia (44.09%), followed by Europe (31.19%), Oceania (24.29%), and North America (19.05%). Multiple mutually exclusive or co-occurring RAS pairs were identified, including Q80K+R155K and R155K+D168G in GT1a and L159F+C316N and R30Q (NS5A)+C316N (NS5B) in GT1b.
CONCLUSION
Our data may be of special relevance for those countries where highly effective antivirals might not be available. Considering the specific RASs prevalence will help the clinicians to make optimal treatment choices. The RASs pairs would benefit anti-HCV drug development.
背景与目的
面对耐药性的直接抗病毒药物(DAA)在世界某些地区仍在使用。因此,确定丙型肝炎病毒(HCV)基因型/亚型以及具有某些常见耐药相关替代(RAS)的位点值得关注。我们调查了所有确诊的HCV亚型(n = 86)中自然发生的RAS的全球和区域频率,并探索了基因、和内以及它们之间同时出现和相互排斥的RAS对。
方法
从NCBI核苷酸数据库中检索截至2019年7月10日可用的总共213,908条HCV序列。经过整理后,对来自未接受过DAA治疗患者的17,312条NS3、8,478条NS5A和25,991条NS5B序列片段进行RAS筛查。使用MEGA 6.0将比对后的核苷酸序列翻译成氨基酸序列,并通过超几何分析确定RAS对。
结果
RAS的流行率在HCV亚型之间有显著差异。例如,对除伏西瑞韦之外的所有蛋白酶抑制剂高度耐药的D168E,在除5a型基因(GT5a)的43.48%序列外的所有亚型中几乎不存在。在NS3中表现出全球分布显著不同的RAS包括1a型基因(GT1a)中的Q80K,在北美频率最高(54.49%),其次是欧洲(26.66%)、亚洲(6.98%)、大洋洲(6.62%)和南美洲(1.03%)。1b型基因(GT1b)中NS3 S122G的流行率在亚洲最高(26.6%),在欧洲最低(2.64%)。1b型基因(GT1b)中的NS5A L28M、R30Q和Y93H,2b型基因(GT2b)中的L31M,以及1b型基因(GT1b)中的NS5B C316N在亚洲最为普遍。与索磷布韦治疗失败相关的3a型基因(GT3a)中的A150V在亚洲最为普遍(44.09%),其次是欧洲(31.19%)、大洋洲(24.29%)和北美(19.05%)。确定了多个相互排斥或同时出现的RAS对,包括1a型基因(GT1a)中的Q80K + R155K和R155K + D168G,以及1b型基因(GT1b)中的L159F + C316N和R30Q(NS5A)+ C316N(NS5B)。
结论
我们的数据可能对那些无法获得高效抗病毒药物的国家具有特殊意义。考虑到特定RAS的流行率将有助于临床医生做出最佳治疗选择。RAS对将有利于抗HCV药物的开发。
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