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PD-1 中的一个意想不到的 N 端环主导了 nivolumab 的结合。

An unexpected N-terminal loop in PD-1 dominates binding by nivolumab.

机构信息

CAS Key Laboratory of Microbial Physiological and Metabolic engineering, Institute of Microbiology, Chinese Academy of Sciences, Beijing 100101, China.

CAS Key Laboratory of Pathogenic Microbiology and Immunology, Institute of Microbiology, Chinese Academy of Sciences, Beijing 100101, China.

出版信息

Nat Commun. 2017 Feb 6;8:14369. doi: 10.1038/ncomms14369.

Abstract

Cancer immunotherapy by targeting of immune checkpoint molecules has been a research 'hot-spot' in recent years. Nivolumab, a human monoclonal antibody targeting PD-1, has been widely used clinically since 2014. However, the binding mechanism of nivolumab to PD-1 has not yet been shown, despite a recent report describing the complex structure of pembrolizumab/PD-1. It has previously been speculated that PD-1 glycosylation is involved in nivolumab recognition. Here we report the complex structure of nivolumab with PD-1 and evaluate the effects of PD-1 N-glycosylation on the interactions with nivolumab. Structural and functional analyses unexpectedly reveal an N-terminal loop outside the IgV domain of PD-1. This loop is not involved in recognition of PD-L1 but dominates binding to nivolumab, whereas N-glycosylation is not involved in binding at all. Nivolumab binds to a completely different area than pembrolizumab. These results provide the basis for the design of future inhibitory molecules targeting PD-1.

摘要

近年来,针对免疫检查点分子的癌症免疫疗法一直是研究的“热点”。自 2014 年以来,针对 PD-1 的人源单克隆抗体纳武单抗已广泛应用于临床。然而,尽管最近有报道描述了派姆单抗/PD-1 的复杂结构,但纳武单抗与 PD-1 的结合机制尚未阐明。此前有研究推测 PD-1 的糖基化参与了纳武单抗的识别。本研究报道了纳武单抗与 PD-1 的复合物结构,并评估了 PD-1 N-糖基化对与纳武单抗相互作用的影响。结构和功能分析出人意料地揭示了 PD-1 IgV 结构域外的一个 N 端环。该环不参与 PD-L1 的识别,但主导与纳武单抗的结合,而 N-糖基化根本不参与结合。纳武单抗与派姆单抗结合的区域完全不同。这些结果为设计针对 PD-1 的未来抑制性分子提供了基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4c9e/5303876/8253bb011fa0/ncomms14369-f1.jpg

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