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一种基于融合机制结构分析的高度稳定的预融合呼吸道合胞病毒F疫苗。

A highly stable prefusion RSV F vaccine derived from structural analysis of the fusion mechanism.

作者信息

Krarup Anders, Truan Daphné, Furmanova-Hollenstein Polina, Bogaert Lies, Bouchier Pascale, Bisschop Ilona J M, Widjojoatmodjo Myra N, Zahn Roland, Schuitemaker Hanneke, McLellan Jason S, Langedijk Johannes P M

机构信息

Janssen Infectious Diseases and Vaccines, Archimedesweg 4-6, Leiden 2333 CN, The Netherlands.

Department of Biochemistry, Geisel School of Medicine at Dartmouth, Hanover, New Hampshire 03755-3844, USA.

出版信息

Nat Commun. 2015 Sep 3;6:8143. doi: 10.1038/ncomms9143.

Abstract

Respiratory syncytial virus (RSV) causes acute lower respiratory tract infections and is the leading cause of infant hospitalizations. Recently, a promising vaccine antigen based on the RSV fusion protein (RSV F) stabilized in the native prefusion conformation has been described. Here we report alternative strategies to arrest RSV F in the prefusion conformation based on the prevention of hinge movements in the first refolding region and the elimination of proteolytic exposure of the fusion peptide. A limited number of unique mutations are identified that stabilize the prefusion conformation of RSV F and dramatically increase expression levels. This highly stable prefusion RSV F elicits neutralizing antibodies in cotton rats and induces complete protection against viral challenge. Moreover, the structural and biochemical analysis of the prefusion variants suggests a function for p27, the excised segment that precedes the fusion peptide in the polypeptide chain.

摘要

呼吸道合胞病毒(RSV)可引起急性下呼吸道感染,是婴儿住院的主要原因。最近,一种基于以天然预融合构象稳定的RSV融合蛋白(RSV F)的有前景的疫苗抗原已被描述。在此,我们报告了基于防止第一个重折叠区域的铰链运动以及消除融合肽的蛋白水解暴露来将RSV F捕获在预融合构象中的替代策略。鉴定出了数量有限的独特突变,这些突变稳定了RSV F的预融合构象并显著提高了表达水平。这种高度稳定的预融合RSV F在棉鼠中引发中和抗体,并诱导对病毒攻击的完全保护。此外,对预融合变体的结构和生化分析表明,p27(多肽链中在融合肽之前切除的片段)具有功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9b2e/4569726/745089578320/ncomms9143-f1.jpg

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