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用编码黄热病毒非结构蛋白NS1、NS2a和NS2b的痘苗病毒重组体免疫小鼠以预防黄热病毒脑炎。

Protection of mice against yellow fever virus encephalitis by immunization with a vaccinia virus recombinant encoding the yellow fever virus non-structural proteins, NS1, NS2a and NS2b.

作者信息

Putnak J R, Schlesinger J J

机构信息

Department of Virus Diseases, Walter Reed Army Institute of Research, Washington, D.C. 20307.

出版信息

J Gen Virol. 1990 Aug;71 ( Pt 8):1697-702. doi: 10.1099/0022-1317-71-8-1697.

Abstract

Recent evidence of a protective immune response to the flavivirus non-structural protein, NS1, has suggested its incorporation into possible recombinant vaccines. The region of the 17D yellow fever virus (YFV) genome encoding the C terminus of envelope glycoprotein and extending to the N terminus of non-structural protein NS3 (NS1-NS2a-NS2b; nucleotides 2030 to 4940) was expressed in vaccinia virus and physical and immunogenic properties of the NS1 moiety were studied. Recombinant NS1 protein, and native YFV NS1, was detected at the surface of infected cells by immunofluorescence and by immune cytolysis after treatment with anti-NS1 antibody and complement. NS1 was also detected in the extracellular medium as a secreted form. Recombinant NS1 was immunoprecipitated as a single protein of approximately the same size as native 17D YFV NS1. Unboiled, both recombinant and native NS1 formed polymers of high Mr. Immunization of mice with this recombinant vaccinia virus stimulated production of non-neutralizing, complement-fixing cytolytic antibody and conferred partial protection against lethal intracerebral inoculation of mice with live 17D YFV.

摘要

最近有证据表明,针对黄病毒非结构蛋白NS1存在保护性免疫反应,这提示可将其用于可能的重组疫苗。编码包膜糖蛋白C端并延伸至非结构蛋白NS3(NS1-NS2a-NS2b;核苷酸2030至4940)N端的17D黄热病毒(YFV)基因组区域在痘苗病毒中表达,并对NS1部分的物理和免疫原性特性进行了研究。通过免疫荧光以及用抗NS1抗体和补体处理后的免疫细胞溶解,在感染细胞表面检测到重组NS1蛋白和天然YFV NS1。NS1在细胞外培养基中也以分泌形式被检测到。重组NS1作为一种大小与天然17D YFV NS1大致相同的单一蛋白被免疫沉淀。未煮沸时,重组NS1和天然NS1均形成高分子量聚合物。用这种重组痘苗病毒免疫小鼠可刺激产生非中和性、补体结合性细胞溶解抗体,并对用活17D YFV进行致死性脑内接种的小鼠提供部分保护。

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