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正黏病毒刺突结构及其中和抗体的识别。

Orthobunyavirus spike architecture and recognition by neutralizing antibodies.

机构信息

Structural Virology Unit, Virology Department, Institut Pasteur, CNRS UMR 3569, 25-28 rue du Dr. Roux, 75015, Paris, France.

Institute of Diagnostic Virology, Friedrich-Loeffler-Institut, Südufer 10, 17493, Greifswald, Insel Riems, Germany.

出版信息

Nat Commun. 2019 Feb 20;10(1):879. doi: 10.1038/s41467-019-08832-8.

Abstract

Orthobunyaviruses (OBVs) form a distinct genus of arthropod-borne bunyaviruses that can cause severe disease upon zoonotic transmission to humans. Antigenic drift or genome segment re-assortment have in the past resulted in new pathogenic OBVs, making them potential candidates for causing emerging zoonoses in the future. Low-resolution electron cryo-tomography studies have shown that OBV particles feature prominent trimeric spikes, but their molecular organization remained unknown. Here we report X-ray crystallography studies of four different OBVs showing that the spikes are formed by an N-terminal extension of the fusion glycoprotein Gc. Using Schmallenberg virus, a recently emerged OBV, we also show that the projecting spike is the major target of the neutralizing antibody response, and provide X-ray structures in complex with two protecting antibodies. We further show that immunization of mice with the spike domains elicits virtually sterilizing immunity, providing fundamental knowledge essential in the preparation for potential newly emerging OBV zoonoses.

摘要

正粘病毒(Orthobunyaviruses,OBVs)是一类独特的节肢动物传播的布尼亚病毒属,在动物源性传播给人类时可导致严重疾病。抗原漂移或基因组片段重组导致过去出现了新的致病性 OBVs,使它们成为未来可能引发新发人畜共患病的潜在候选者。低分辨率电子 cryo-tomography 研究表明,OBV 颗粒具有明显的三聚体刺突,但它们的分子结构仍不清楚。本研究报告了对四种不同 OBVs 的 X 射线晶体学研究,表明刺突是由融合糖蛋白 Gc 的 N 端延伸形成的。我们还使用最近出现的 OBV Schmallenberg 病毒表明,突出的刺突是中和抗体反应的主要靶标,并提供了与两种保护抗体结合的 X 射线结构。我们进一步表明,用刺突结构域免疫小鼠可产生几乎完全的免疫,为应对潜在新发 OBV 人畜共患病提供了必要的基础知识。

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