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针对黄热病毒(YF)包膜蛋白的保护性单克隆抗体的中和性F(ab')2片段无法保护小鼠免受致死性YF脑炎的侵害。

Neutralizing F(ab')2 fragments of protective monoclonal antibodies to yellow fever virus (YF) envelope protein fail to protect mice against lethal YF encephalitis.

作者信息

Schlesinger J J, Chapman S

机构信息

University of Rochester School of Medicine & Dentistry, NY 14621.

出版信息

J Gen Virol. 1995 Jan;76 ( Pt 1):217-20. doi: 10.1099/0022-1317-76-1-217.

DOI:10.1099/0022-1317-76-1-217
PMID:7844536
Abstract

Monoclonal antibodies (MAbs) prepared against the yellow fever virus (YF) vaccine strain 17D (17D YF) envelope E protein were used to investigate Fc piece involvement in antibody-mediated protection against YF encephalitis in mice 17D YF passaged either in Vero cells or in mouse brain (P-YF) to increase neurovirulence was used. To avoid uncertainty concerning antibody clearance and blood-brain barrier penetration, and to directly compare protective activity with neutralization in vitro, pre-formed antibody-virus complexes were injected intracerebrally or assayed for plaque formation in parallel. F(ab')2 fragments of an IgG2a MAb that strongly neutralized both YF strains retained molar equivalent neutralizing activity in vitro, but did not protect. However, further incubation of such F(ab')2-virus antibody complexes with rabbit IgG, but not F(ab')2 anti-mouse IgG resulted in protection. To unambiguously test for Fc piece involvement in this model we derived an IgG2a isotype switch variant from a protective IgG1 MAb-secreting hybridoma and prepared F(ab')2 fragments of the derivative. Intact and fragmented antibodies exhibited weak neutralizing activity. The variant antibody failed to protect against P-YF, but against considerably less neurovirulent 17D YF its protective capacity was 10-fold higher than that of its IgG1 parent. F(ab')2 fragments of the variant did not protect. Together, these results provide strong evidence of an in vivo protective function for the anti-virion antibody Fc piece and indicate that in vitro neutralizing activity as a predictor of antibody protective capacity is dependent on Fc piece integrity and isotype.

摘要

制备了针对黄热病毒(YF)疫苗株17D(17D YF)包膜E蛋白的单克隆抗体(MAb),用于研究Fc片段在抗体介导的小鼠抗YF脑炎保护中的作用。使用在Vero细胞或小鼠脑中传代(P - YF)以增加神经毒力的17D YF。为避免抗体清除和血脑屏障穿透方面的不确定性,并直接将保护活性与体外中和作用进行比较,预先形成的抗体 - 病毒复合物通过脑内注射或并行进行蚀斑形成测定。一种强烈中和两种YF毒株的IgG2a MAb的F(ab')2片段在体外保留了摩尔当量的中和活性,但没有保护作用。然而,将这种F(ab')2 - 病毒抗体复合物与兔IgG进一步孵育,而不是与F(ab')2抗小鼠IgG孵育,会产生保护作用。为了明确测试该模型中Fc片段的作用,我们从分泌保护性IgG1 MAb的杂交瘤中获得了IgG2a同种型转换变体,并制备了衍生物的F(ab')2片段。完整和片段化的抗体表现出较弱的中和活性。该变体抗体不能保护小鼠免受P - YF感染,但对于神经毒力明显较低的17D YF,其保护能力比其IgG1亲本高10倍。该变体的F(ab')2片段没有保护作用。总之,这些结果为抗病毒抗体Fc片段的体内保护功能提供了有力证据,并表明体外中和活性作为抗体保护能力的预测指标取决于Fc片段的完整性和同种型。

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