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Differential reactivity of mouse monoclonal anti-HBs antibodies with recombinant mutant HBs antigens.

机译:小鼠单克隆抗HBs抗体与重组突变HBs抗原的差异反应性。

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AIM: To investigate the reactivity of a panel of 8 mouse anti-hepatitis B surface antigen (HBsAg) monoclonal antibodies (mAbs) using a collection of 9 recombinant HBsAg mutants with a variety of amino acid substitutions mostly located within the "a" region. METHODS: The entire HBs genes previously cloned into a mammalian expression vector were transiently transfected into COS7 cells. Two standard unmutated sequences of the ayw and adw subtypes served as controls. Secreted mutant proteins were collected and measured by three commercial diagnostic immunoassays to assess transfection efficiency. Reactivity of anti-HBs mAbs with mutated HBsAgs was determined by sandwich enzyme-linked immunosorbent assay (ELISA). RESULTS: Reactivity of anti-HBs mAbs with mutated HBsAgs revealed different patterns. While three mutants reacted strongly with all mAbs, two mutants reacted weakly with only two mAbs and the remaining proteins displayed variable degrees of reactivity towards different mAbs. Accordingly, four groups of mAbs with different but overlapping reactivity patterns could be envisaged. One group consisting of two mAbs (37C5-S7 and 35C6-S11) was found to recognize stable linear epitopes conserved in all mutants. Mutations outside the "a" determinant at positions 120 (P-->S), 123(T-->N) and 161 (M-->T) were found to affect reactivity of these mAbs. CONCLUSION: Our findings could have important implications for biophysical studies, vaccination strategies and immunotherapy of hepatitis B virus (HBV) mutants.
机译:目的:使用9种重组HBsAg突变体的集合来调查一组8种小鼠抗乙型肝炎表面抗原(HBsAg)单克隆抗体(mAbs)的反应性,这些突变体大多位于“ a”区内,具有多种氨基酸取代。方法:将先前克隆到哺乳动物表达载体中的全部HBs基因瞬时转染到COS7细胞中。 ayw和adw亚型的两个标准未突变序列用作对照。收集分泌的突变蛋白并通过三种商业诊断性免疫测定法进行评估,以评估转染效率。通过夹心酶联免疫吸附测定(ELISA)测定抗HBs mAb与突变HBsAg的反应性。结果:抗HBs mAb与HBsAg突变的反应性显示出不同的模式。尽管三个突变体均与所有mAb发生强烈反应,但两个突变体仅与两个mAb发生微弱反应,其余蛋白质对不同mAb表现出不同程度的反应性。因此,可以设想四组具有不同但重叠的反应模式的mAb。发现由两个mAb(37C5-S7和35C6-S11)组成的一组识别所有突变体中保守的稳定线性表位。发现在位置120(P-> S),123(T-> N)和161(M-> T)的“ a”行列式之外的突变会影响这些mAb的反应性。结论:我们的发现可能对乙型肝炎病毒(HBV)突变体的生物物理研究,疫苗接种策略和免疫疗法具有重要意义。

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