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痘苗病毒进入/融合复合体亚基A28是中和性及保护性抗体的靶点。

Vaccinia virus entry/fusion complex subunit A28 is a target of neutralizing and protective antibodies.

作者信息

Nelson Gretchen E, Sisler Jerry R, Chandran Dev, Moss Bernard

机构信息

Laboratory of Viral Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892-3210, USA.

出版信息

Virology. 2008 Oct 25;380(2):394-401. doi: 10.1016/j.virol.2008.08.009. Epub 2008 Sep 11.

DOI:10.1016/j.virol.2008.08.009
PMID:18789472
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2628551/
Abstract

The vaccinia virus entry/fusion complex (EFC) is comprised of at least eight transmembrane proteins that are conserved in all poxviruses. However, neither the physical structure of the EFC nor the immunogenicity of the individual components has been determined. We prepared soluble forms of two EFC components, A28 and H2, by replacing the transmembrane domain with a signal peptide and adding a polyhistidine tail. The proteins were expressed by baculoviruses, secreted from insect cells, purified by affinity chromatography and used to raise antibodies in rabbits. The antibodies recognized the viral proteins but only the antibody to recombinant A28 bound intact virions and neutralized infectivity. Analyses with a set of overlapping peptides revealed a neutralizing epitope between residues 73 and 92 of A28. Passive immunization of mice with IgG purified from the anti-A28 serum provided partial protection against a vaccinia virus intranasal challenge, whereas IgG from the anti-H2 serum did not.

摘要

痘苗病毒进入/融合复合体(EFC)由至少八种跨膜蛋白组成,这些蛋白在所有痘病毒中都是保守的。然而,EFC的物理结构和各个组分的免疫原性均未确定。我们通过用信号肽取代跨膜结构域并添加多聚组氨酸尾巴,制备了两种EFC组分A28和H2的可溶性形式。这些蛋白由杆状病毒表达,从昆虫细胞中分泌出来,通过亲和层析纯化,并用于在兔体内产生抗体。这些抗体识别病毒蛋白,但只有抗重组A28的抗体能结合完整病毒粒子并中和感染性。用一组重叠肽进行分析揭示了A28第73至92位残基之间的一个中和表位。用从抗A28血清中纯化的IgG对小鼠进行被动免疫,可提供部分保护以抵抗痘苗病毒鼻内攻击,而来自抗H2血清的IgG则不能。

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