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Characterization of potential antiviral resistance mutations in hepatitis B virus reverse transcriptase sequences in treatment-naive Chinese patients.

机译:初治中国患者乙型肝炎病毒逆转录酶序列中潜在抗病毒耐药性突变的特征。

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Full-length hepatitis B virus (HBV) reverse transcriptase (RT) sequences were amplified and sequenced among 192 nucleos(t)ide analogue (NA)-naive Chinese patients with chronic hepatitis B. Deduced amino acids (AAs) at 42 previously reported potential NA resistance (NAr) mutation positions in RT region were analyzed. Patients were found with either B-genotype (28.65%) or C-genotype (71.35%) infections. Rt53, rt91, rt124, rt134, rt221, rt224, rt238 and rt256 were identified as B- and C-genotype-dependent polymorphic AA positions. AA substitutions at 11 classical NAr mutation positions, i.e. rt80, rt169, rt173, rt180, rt181, rt184, rt194, rt202, rt204, rt236 and rt250, were not detected. However, potential NAr mutations were found in 30.73% (59/192) isolates, which involved 18 positions including rt53, rt207, rt229, rt238 and rt256, etc. The concomitant AA changes of HBsAg occurred in 16.67% (32/192) isolates including sG145R mutation. One-third of mutation positions were located in functional RT domains (e.g. rt207 and rt233), A-B interdomains (overlapping HBsAg 'a' determinant and showing most concomitant immune-associated mutations) and non-A-B interdomains (e.g. rt191 and rt213), respectively. Genotypes B and C each showed several preferred positions to mutate. These results might provide insights into understanding the evolution and selection basis of NAr HBV strains under antiviral therapy.
机译:在192名无核苷酸(NA)的中国慢性乙型肝炎患者中扩增了全长乙型肝炎病毒(HBV)逆转录酶(RT)序列,并进行了测序。先前报道的42种可能的推导氨基酸(AAs)分析了RT区域中的NA抗性(NAr)突变位置。发现患者患有B基因型(28.65%)或C基因型(71.35%)感染。 Rt53,rt91,rt124,rt134,rt221,rt224,rt238和rt256被确定为B和C基因型依赖的多态AA位置。未检测到11个经典NAr突变位置(即rt80,rt169,rt173,rt180,rt181,rt184,rt194,rt202,rt204,rt236和rt250)的AA取代。但是,在30.73%(59/192)分离株中发现了潜在的NAr突变,其中包括rt53,rt207,rt229,rt238和rt256等18个位置。HBsAg的伴随AA变化发生在16.67%(32/192)分离株中。包括sG145R突变。突变位置的三分之一分别位于功能性RT域(例如rt207和rt233),AB间域(重叠HBsAg'a'决定簇并显示出大多数伴随的免疫相关突变)和非AB间域(例如rt191和rt213)。 。基因型B和C均显示出几个优选的突变位置。这些结果可能为了解抗病毒治疗的NAr HBV菌株的进化和选择基础提供见识。

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