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作为广泛中和抗体靶点的HIV聚糖屏蔽层

The HIV glycan shield as a target for broadly neutralizing antibodies.

作者信息

Doores Katie J

机构信息

Department of Infectious Diseases, Faculty of Life Sciences and Medicine, King's College London, Guy's Hospital, UK.

出版信息

FEBS J. 2015 Dec;282(24):4679-91. doi: 10.1111/febs.13530. Epub 2015 Oct 23.

Abstract

The HIV envelope glycoprotein (Env) is the sole target for HIV broadly neutralizing antibodies (bnAbs). HIV Env is one of the most heavily glycosylated proteins known, with approximately half of its mass consisting of host-derived N-linked glycans. The high density of glycans creates a shield that impedes antibody recognition but, critically, some of the most potent and broadly active bnAbs have evolved to recognize epitopes formed by these glycans. Although the virus hijacks the host protein synthesis and glycosylation machinery to generate glycosylated HIV Env, studies have shown that HIV Env glycosylation diverges from that typically observed on host-derived glycoproteins. In particular, the high density of glycans leads to a nonself motif of underprocessed oligomannose-type glycans that forms the target of some of the most broad and potent HIV bnAbs. This review discusses the changing perception of the HIV glycan shield, and summarizes the protein-directed and cell-directed factors controlling HIV Env glycosylation that impact on HIV bnAb recognition and HIV vaccine design strategies.

摘要

HIV包膜糖蛋白(Env)是HIV广谱中和抗体(bnAbs)的唯一靶点。HIV Env是已知糖基化程度最高的蛋白质之一,其质量约一半由宿主来源的N-连接聚糖组成。高密度的聚糖形成了一个屏障,阻碍抗体识别,但关键的是,一些最有效且具有广泛活性的bnAbs已经进化到能够识别由这些聚糖形成的表位。尽管病毒劫持宿主蛋白质合成和糖基化机制以产生糖基化的HIV Env,但研究表明,HIV Env糖基化与宿主来源糖蛋白上通常观察到的情况不同。特别是,高密度的聚糖导致了加工不足的寡甘露糖型聚糖的非自身基序,这构成了一些最广泛和有效的HIV bnAbs的靶点。本综述讨论了对HIV聚糖屏障不断变化的认识,并总结了控制HIV Env糖基化的蛋白质导向和细胞导向因素,这些因素影响HIV bnAb识别和HIV疫苗设计策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9be6/4950053/cb4fcf33d078/FEBS-282-4679-g001.jpg

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