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寨卡病毒包膜蛋白聚糖环调节病毒体抗原性。

The Zika virus envelope protein glycan loop regulates virion antigenicity.

作者信息

Goo Leslie, DeMaso Christina R, Pelc Rebecca S, Ledgerwood Julie E, Graham Barney S, Kuhn Richard J, Pierson Theodore C

机构信息

Viral Pathogenesis Section, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD, United States of America.

Vaccine Research Center, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD, USA.

出版信息

Virology. 2018 Feb;515:191-202. doi: 10.1016/j.virol.2017.12.032. Epub 2018 Jan 2.

Abstract

Because antibodies are an important component of flavivirus immunity, understanding the antigenic structure of flaviviruses is critical. Compared to dengue virus (DENV), the loop containing the single N-linked glycosylation site on Zika virus (ZIKV) envelope (E) proteins extends further towards the DII fusion loop (DII-FL) on neighboring E proteins within E dimers on mature viruses. Although ZIKV is poorly neutralized by DII-FL antibodies, we demonstrated significantly increased neutralization sensitivity of ZIKV particles incorporating the DENV glycan loop. Increased neutralization sensitivity was independent of E protein glycosylation: ZIKV lacking E protein glycans remained poorly neutralized, whereas ZIKV loop chimeras with or without an E protein glycan were potently neutralized. ZIKV particles lacking the E protein glycan were capable of infecting Raji cells expressing the lectin DC-SIGNR, suggesting the prM glycan of partially mature particles can facilitate entry. Our study provides insight into the determinants of ZIKV E protein function and antigenicity.

摘要

由于抗体是黄病毒免疫的重要组成部分,了解黄病毒的抗原结构至关重要。与登革病毒(DENV)相比,寨卡病毒(ZIKV)包膜(E)蛋白上含有单个N-连接糖基化位点的环向成熟病毒E二聚体内相邻E蛋白上的DII融合环(DII-FL)延伸得更远。尽管ZIKV很难被DII-FL抗体中和,但我们证明,掺入DENV聚糖环的ZIKV颗粒的中和敏感性显著增加。中和敏感性的增加与E蛋白糖基化无关:缺乏E蛋白聚糖的ZIKV仍然很难被中和,而带有或不带有E蛋白聚糖的ZIKV环嵌合体则能被有效中和。缺乏E蛋白聚糖的ZIKV颗粒能够感染表达凝集素DC-SIGNR的Raji细胞,这表明部分成熟颗粒的prM聚糖可以促进病毒进入。我们的研究为了解ZIKV E蛋白功能和抗原性的决定因素提供了见解。

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