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从感染中分泌的登革热病毒 NS1 主要是二聚体,并与高密度脂蛋白结合。

Secreted dengue virus NS1 from infection is predominantly dimeric and in complex with high-density lipoprotein.

机构信息

Lee Kong Chian School of Medicine, Nanyang Technological University, Singapore, Singapore.

NTU Institute of Structural Biology, Nanyang Technological University, Singapore, Singapore.

出版信息

Elife. 2024 May 24;12:RP90762. doi: 10.7554/eLife.90762.

DOI:10.7554/eLife.90762
PMID:38787378
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11126310/
Abstract

Severe dengue infections are characterized by endothelial dysfunction shown to be associated with the secreted nonstructural protein 1 (sNS1), making it an attractive vaccine antigen and biotherapeutic target. To uncover the biologically relevant structure of sNS1, we obtained infection-derived sNS1 (isNS1) from dengue virus (DENV)-infected Vero cells through immunoaffinity purification instead of recombinant sNS1 (rsNS1) overexpressed in insect or mammalian cell lines. We found that isNS1 appeared as an approximately 250 kDa complex of NS1 and ApoA1 and further determined the cryoEM structures of isNS1 and its complex with a monoclonal antibody/Fab. Indeed, we found that the major species of isNS1 is a complex of the NS1 dimer partially embedded in a high-density lipoprotein (HDL) particle. Crosslinking mass spectrometry studies confirmed that the isNS1 interacts with the major HDL component ApoA1 through interactions that map to the NS1 wing and hydrophobic domains. Furthermore, our studies demonstrated that the sNS1 in sera from DENV-infected mice and a human patient form a similar complex as isNS1. Our results report the molecular architecture of a biological form of sNS1, which may have implications for the molecular pathogenesis of dengue.

摘要

重症登革热感染的特征是内皮功能障碍,据表明与分泌的非结构蛋白 1(sNS1)有关,这使其成为有吸引力的疫苗抗原和生物治疗靶标。为了揭示 sNS1 的生物学相关结构,我们通过免疫亲和纯化从登革病毒(DENV)感染的 Vero 细胞中获得感染衍生的 sNS1(isNS1),而不是在昆虫或哺乳动物细胞系中过表达重组 sNS1(rsNS1)。我们发现 isNS1 表现为大约 250 kDa 的 NS1 和 ApoA1 复合物,并且进一步确定了 isNS1 及其与单克隆抗体/Fab 的复合物的 cryoEM 结构。实际上,我们发现 isNS1 的主要形式是部分嵌入高密度脂蛋白(HDL)颗粒中的 NS1 二聚体复合物。交联质谱研究证实,isNS1 通过与 NS1 翼和疏水区映射的相互作用与主要的 HDL 成分 ApoA1 相互作用。此外,我们的研究表明,来自 DENV 感染小鼠和人类患者血清中的 sNS1 形成与 isNS1 相似的复合物。我们的研究结果报告了 sNS1 的一种生物学形式的分子结构,这可能对登革热的分子发病机制具有重要意义。

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