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SIV 感染持续时间在很大程度上决定了猕猴中和抗体反应的拓宽。

SIV infection duration largely determines broadening of neutralizing antibody response in macaques.

机构信息

Shanghai Public Health Clinical Center, Fudan University, Shanghai, China.

Laboratory of Molecular Microbiology, National Institute of Allergy and Infectious Diseases (NIAID), NIH, Bethesda, Maryland, USA.

出版信息

J Clin Invest. 2020 Oct 1;130(10):5413-5424. doi: 10.1172/JCI139123.

Abstract

The development of broadly neutralizing antibodies (BNAbs) in HIV infection is a result of long-term coevolutionary interaction between viruses and antibodies. Understanding how this interaction promotes the increase of neutralization breadth during infection will improve the way in which AIDS vaccine strategies are designed. In this paper, we used SIV-infected rhesus macaques as a model to study the development of neutralization breadth by infecting rhesus macaques with longitudinal NAb escape variants and evaluating the kinetics of NAb response and viral evolution. We found that the infected macaques developed a stepwise NAb response against escape variants and increased neutralization breadth during the course of infection. Furthermore, the increase of neutralization breadth correlated with the duration of infection but was independent of properties of the inoculum, viral loads, or viral diversity during infection. These results imply that the duration of infection was the main factor driving the development of BNAbs. These data suggest the importance of novel immunization strategies to induce effective NAb response against HIV infection by mimicking long-term infection.

摘要

HIV 感染中广谱中和抗体(BNAbs)的发展是病毒和抗体之间长期共同进化相互作用的结果。了解这种相互作用如何促进感染过程中中和广度的增加,将改善艾滋病疫苗策略的设计方式。在本文中,我们使用 SIV 感染的恒河猴作为模型,通过感染恒河猴的纵向 NAb 逃逸变异体来研究中和广度的发展,并评估 NAb 反应和病毒进化的动力学。我们发现,感染的猕猴针对逃逸变体逐渐产生了 NAb 反应,并在感染过程中增加了中和广度。此外,中和广度的增加与感染持续时间相关,但与接种物的特性、病毒载量或感染过程中的病毒多样性无关。这些结果表明,感染持续时间是驱动 BNAbs 发展的主要因素。这些数据表明,通过模拟长期感染,诱导针对 HIV 感染的有效 NAb 反应的新型免疫策略的重要性。

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