首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Rapid development of glycan-specific broad and potent anti–HIV-1 gp120 neutralizing antibodies in an R5 SIV/HIV chimeric virus infected macaque
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Rapid development of glycan-specific broad and potent anti–HIV-1 gp120 neutralizing antibodies in an R5 SIV/HIV chimeric virus infected macaque

机译:R5 SIV / HIV嵌合病毒感染的猕猴中聚糖特异性广泛而有效的抗HIV-1 gp120中和抗体的快速开发

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摘要

It is widely believed that the induction of a broadly neutralizing antibody (bNAb) response will be a critical component of a successful vaccine against HIV. A significant fraction of HIV-infected individuals mount bNAb responses, providing support for the notion that such responses could be elicited through vaccination. Infection of macaques with simian immunodeficiency virus (SIV) or SIV/HIV chimeric virus (SHIV) has been widely used to model aspects of HIV infection, but to date, only limited bNAb responses have been described. Here, we screened plasma from 14 R5-tropic SHIV-infected macaques for broadly neutralizing activity and identified a macaque with highly potent cross-clade plasma NAb response. Longitudinal studies showed that the development of broad and autologous NAb responses occurred coincidentally in this animal. Serum-mapping studies, using pseudovirus point mutants and antigen adsorption assays, indicated that the plasma bNAbs are specific for epitopes that include carbohydrates and are critically dependent on the glycan at position 332 of Env gp120. The results described herein provide insight into the development and evolution of a broad response, suggest that certain bNAb specificities may be more rapidly induced by immunization than others, and provide a potential model for the facile study of the development of bNAb responses.
机译:普遍认为,广泛中和抗体(bNAb)应答的诱导将是成功的抗HIV疫苗的关键组成部分。感染HIV的个体中有很大一部分发起了bNAb反应,从而支持了可以通过疫苗接种引发这种反应的观点。猿猴免疫缺陷病毒(SIV)或SIV / HIV嵌合病毒(SHIV)感染猕猴已被广泛用于模拟HIV感染,但迄今为止,仅描述了有限的bNAb反应。在这里,我们从14个R5嗜SHIV感染的猕猴中筛选了具有广泛中和活性的血浆,并鉴定了具有高效交叉血浆血浆NAb反应的猕猴。纵向研究表明,这种动物同时发生广泛的自体NAb反应。使用伪病毒点突变体和抗原吸附测定法进行的血清图谱研究表明,血浆bNAb对包括碳水化合物的表位具有特异性,并严重依赖于Env gp120 332位的聚糖。本文所述的结果提供了对广泛应答的发生和发展的洞察力,表明某些bNAb特异性可能比其他应答更快速地被免疫诱导,并为轻松研究bNAb应答的发生提供了潜在的模型。

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