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Anti-HIV-1 antibody-dependent cellular cytotoxicity: is there more to antibodies than neutralization?

机译:抗HIV-1抗体依赖性细胞细胞毒性:是否有更多的抗体比中和?

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Purpose of review An increasing body of evidence suggests that nonneutralizing Fc effector functions including antibody-dependent cellular cytotoxicity (ADCC) contribute to protection against HIV-1 acquisition. We discuss recent advances in anti-HIV-1 ADCC research with a particular focus on ADCC mediated by Env-specific antibodies in vitro and in vivo , the curative potential of HIV-1-specific ADCC antibodies and the mechanisms of HIV-1 resistance to ADCC. Recent findings ADCC activities of broadly neutralizing and nonneutralizing monoclonal antibody panels were recently characterized in vitro against several lab-adapted and primary isolates of HIV-1. ADCC activity of these monoclonal antibodies generally correlated with binding to infected cells and were greater against the lab-adapted strains compared with primary HIV-1 isolates. Several recent studies in mouse and macaque models of HIV-1 infection suggest Fc-mediated effector functions contribute to the protective efficacy of broadly neutralizing antibodies and exert immune pressure on HIV-1 in vivo . Summary An increasing body of evidence suggests that ADCC-mediating antibodies, particularly when combined with neutralizing functions, can facilitate prevention and control of HIV-1. The precise mechanisms of partial protection conferred by nonneutralizing antibodies in vivo remain unclear and will need to be fully investigated in order to realize their full potential for HIV-1 vaccines.
机译:审查目的的目的,增加的证据表明,非暴力的FC效应功能包括依赖于依赖性细胞细胞毒性(ADCC)有助于防止HIV-1收购。我们讨论了抗HIV-1 ADCC研究的最新进展,特别关注了体外鉴定的eng特异性抗体介导的ADCC,HIV-1特异性ADCC抗体的疗效和HIV-1耐受机制ADCC。最近发现ADCC的宽度中和和非线性的单克隆抗体面板的活性在体外对几种实验室适应的HIV-1的初级分离株进行了体外。与初级HIV-1分离株相比,这些单克隆抗体的adcc活性与与感染细胞的结合相关,并且与实验室适应的菌株更大。最近在HIV-1感染的小鼠和猕猴模型中的几项研究表明FC介导的效应功能有助于广泛中和抗体的保护效果,并在体内对HIV-1施加免疫压力。发明内容越来越多的证据表明ADCC介导的抗体,特别是当与中和功能结合时,可以促进预防和控制HIV-1。在体内非线上和抗体赋予的局部保护的精确机制仍然不清楚,需要完全研究,以实现其HIV-1疫苗的全部潜力。

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