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首页> 外文期刊>Journal of Hepatology: The Journal of the European Association for the Study of the Liver >Influence of mutations in hepatitis B virus surface protein on viral antigenicity and phenotype in occult HBV strains from blood donors
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Influence of mutations in hepatitis B virus surface protein on viral antigenicity and phenotype in occult HBV strains from blood donors

机译:乙型肝炎病毒表面蛋白突变对献血者隐匿性HBV株病毒抗原性和表型的影响

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Background & Aims: This study aimed at investigating mutations in the hepatitis B surface protein (HBsAg) in occult hepatitis B virus (HBV) infection (OBI) and their influence on viral antigenicity and phenotype. Methods: The characteristics of 61 carriers with OBI (OBI group), 153 HBsAg(+) carriers with serum HBsAg ≤100 IU/ml (HBsAg-L group) and 54 carriers with serum HBsAg >100 IU/ml (HBsAg-H group) from 38,499 blood donors were investigated. Mutations in the major hydrophilic region (MHR) of the viral sequences were determined. Thirteen representative MHR mutations observed in OBI sequences were antigenically characterized with a panel of monoclonal antibodies (MAbs) and commercial HBsAg immunoassays and functionally characterized in HuH7 cells and hydrodynamically injected mice. Results: Of 61 OBI sequences, 34 (55.7%) harbored MHR mutations, which was significantly higher than the frequency in either the HBsAg-L (34.0%, p = 0.003) or the HBsAg-H group (17.1%, p <0.001). Alterations in antigenicity induced by the 13 representative MHR mutations identified in the OBI group were assessed by reacting recombinant HBV mutants with 30 different MAbs targeting various epitopes. Four out of the 13 mutations (C124R, C124Y, K141E, and D144A) strongly decreased the analytical sensitivity of seven commercial HBsAg immunoassays, and 10 (G119R, C124Y, I126S, Q129R, S136P, C139R, T140I, K141E, D144A, and G145R) significantly impaired virion and/or S protein secretion in both HuH7 cells and mice. Conclusions: MHR mutations alter antigenicity and impair virion secretion, both of which may contribute to HBsAg detection failure in individuals with OBI.
机译:背景与目的:这项研究旨在调查隐匿性乙型肝炎病毒(HBV)感染(OBI)中的乙型肝炎表面蛋白(HBsAg)突变及其对病毒抗原性和表型的影响。方法:61名OBI携带者(OBI组),153名HBsAg≤100IU / ml的HBsAg(+)携带者(HBsAg-L组)和54例HBsAg> 100 IU / ml的携带者(HBsAg-H组)的特征)对38,499名献血者进行了调查。确定了病毒序列的主要亲水区(MHR)中的突变。在OBI序列中观察到的13个代表性MHR突变通过一系列单克隆抗体(MAb)和商业HBsAg免疫测定进行抗原表征,并在HuH7细胞和水动力注射小鼠中进行功能表征。结果:在61个OBI序列中,有34个(55.7%)带有MHR突变,明显高于HBsAg-L(34.0%,p = 0.003)或HBsAg-H组的频率(17.1%,p <0.001 )。通过使重组HBV突变体与30种靶向各种表位的单克隆抗体反应,来评估OBI组中鉴定出的13种代表性MHR突变诱导的抗原性变化。 13种突变中的4种(C124R,C124Y,K141E和D144A)大大降低了7种商业HBsAg免疫测定的分析灵敏度,另外10种(G119R,C124Y,I126S,Q129R,S136P,C139R,T140I,K141E,D144A和G145R )大大削弱了HuH7细胞和小鼠的病毒体和/或S蛋白的分泌。结论:MHR突变会改变抗原性并损害病毒颗粒分泌,这两者都可能导致OBI患者的HBsAg检测失败。

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