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首页> 外文期刊>Virology >Dengue virus neutralization is modulated by IgG antibody subclass and Fcgamma receptor subtype.
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Dengue virus neutralization is modulated by IgG antibody subclass and Fcgamma receptor subtype.

机译:登革病毒的中和受IgG抗体亚类和Fcgamma受体亚型调节。

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摘要

Severe dengue virus (DENV) infection is epidemiologically linked to pre-existing anti-DENV antibodies acquired by maternal transfer or primary infection. A possible explanation is that DENV immune complexes evade neutralization by engaging Fcgamma receptors (FcgammaR) on monocytes, natural targets for DENV in humans. Using epitope-matched humanized monoclonal antibodies (mAbs) and stable FcgammaR-transfected CV-1 cells, we found that DENV neutralization by IgG1, IgG3, and IgG4 mAbs was enhanced in high-affinity FcgammaRIA transfectants and diminished in low-affinity FcgammaRIIA transfectants, whereas neutralization by IgG2 mAbs (low-affinity ligands for both FcgammaRs) was diminished equally. In FcgammaR-negative Vero cells, IgG3 mAbs exhibited the strongest neutralizing activity and IgG2, the weakest. Our results demonstrate that DENV neutralization is modulated by the Fc region in an IgG subclass manner, likely through effects on virion and FcgammaR binding. Thus, the IgG antibody subclass profile generated by DENV infection or vaccination may independently influence the magnitude of the neutralizing response.
机译:严重的登革热病毒(DENV)感染在流行病学上与通过母体转移或原发性感染获得的预先存在的抗DENV抗体相关。可能的解释是,DENV免疫复合物通过使单核细胞上的Fcgamma受体(FcgammaR)参与人DENV的天然靶标而逃避中和。使用表位匹配的人源化单克隆抗体(mAb)和稳定的FcgammaR转染的CV-1细胞,我们发现IgG1,IgG3和IgG4 mAb的DENV中和作用在高亲和力FcgammaRIA转染子中得到增强,而在低亲和力FcgammaRIIA转染子中被减弱,而IgG2 mAb(两个FcgammaR的低亲和力配体)的中和作用则平均降低。在FcgammaR阴性Vero细胞中,IgG3 mAb表现出最强的中和活性,而IgG2最弱。我们的结果表明,DENV中和作用可能是通过对病毒体和FcgammaR结合的影响而以IgG亚类的方式由Fc区调节的。因此,由DENV感染或疫苗接种产生的IgG抗体亚类概况可独立影响中和反应的强度。

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