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HIV therapy by a combination of broadly neutralizing antibodies in humanized mice

机译:通过在人源化小鼠中广泛中和抗体的组合进行HIV治疗

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摘要

Human antibodies to human immunodeficiency virus-1 (HIV-1) can neutralize a broad range of viral isolates in vitro and protect non-human primates against infection. Previous work showed that antibodies exert selective pressure on the virus but escape variants emerge within a short period of time. However, these experiments were performed before the recent discovery of more potent anti-HIV-1 antibodies and their improvement by structure-based design. Here we re-examine passive antibody transfer as a therapeutic modality in HIV-1-infected humanized mice. Although HIV-1 can escape from antibody monotherapy, combinations of broadly neutralizing antibodies can effectively control HIV-1 infection and suppress viral load to levels below detection. Moreover, in contrast to antiretroviral therapy the longer half-life of antibodies led to control of viraemia for an average of 60 days after cessation of therapy. Thus, combinations of potent monoclonal antibodies can effectively control HIV-1 replication in humanized mice, and should be re-examined as a therapeutic modality in HIV-1-infected individuals.
机译:抗人类免疫缺陷病毒1(HIV-1)的人类抗体可以在体外中和广泛的病毒分离株,并保护非人类灵长类动物免受感染。先前的工作表明,抗体对病毒施加选择性压力,但在短时间内会出现逃脱变体。但是,这些实验是在最近发现更有效的抗HIV-1抗体及其通过基于结构的设计进行改进之前进行的。在这里,我们重新检查被动抗体转移作为HIV-1感染的人源化小鼠的治疗方式。尽管HIV-1可以从抗体单一疗法中逃脱,但广泛中和抗体的组合可以有效控制HIV-1感染并将病毒载量抑制到检测不到的水平。此外,与抗逆转录病毒疗法相比,抗体的半衰期更长,可在停止治疗后平均控制病毒血症60天。因此,有效的单克隆抗体的组合可以有效地控制人源化小鼠中的HIV-1复制,应该作为HIV-1感染者的治疗方式进行重新检查。

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