Measles virus-specific immunoglobulin G subclass response in serum and cerebrospinal fluid

Mitsuo Narita, Satoshi Yamada, Yoshihiro Matsuzono, Osamu Itakura, Takehiro Togashi , Hideaki Kikuta
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引用次数: 15

Abstract

Background: While many previous studies have focused on the impairment in the cellular immunity during measles virus infection, to date, a limited amount of data is available concerning the virus-specific IgG subclass response during measles virus infection.

Objective: The purpose of this study is to analyze the measles virus infection on the basis of virus-specific IgG subclass (G 1 and G 3).

Study design: Frozen-stored, serum and/or cerebospinal fluid samples from three groups of patients were tested retrospectively; Group 1 comprised 14 patients with measles primary infection, group 2, ten patients with reinfection/vaccine failure, and group 3, seven patients with subacute sclerosing panencephalitis. The method used was a modified ELISA method utilizing the Enzygnost IgG detection kit with mouse-monoclonal antibodies (clone HP6091 for IgG 1 and clone HP6050 for IgG 3). Avidity testing for each subclass IgG was also performed for selected samples by means of an 8 M urea-denaturation method.

Results: In group 1, the IgG 3 could be detected in serum within 7 days from the onset of rash more frequently than IgG 1. In the cases of group 2, both subclasses were detected in very acute phase serum samples. In these cases, the IgG 1-specific avidity was always higher than that of IgG 3. In group 3, the subclass IgGs detected in the cerebrospinal fluid had a lower avidity than those in the serum.

Conclusions: Our results suggested that in measles virus infection, like other viral infections, the IgG 3 response normally occurs before the IgG 1 response, and plays a major role in the acute phase immunity during the primary infection, while the IgG 1 plays a major role in the maintenance of immunity. Continuously produced IgG 1 and IgG 3 in the central nervous system in cases of subacute sclerosing panencephalitis may be derived from cell populations different from those in the blood.

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麻疹病毒特异性免疫球蛋白G亚类在血清和脑脊液中的反应
背景:虽然以前的许多研究都集中在麻疹病毒感染期间细胞免疫功能的损害,但迄今为止,关于麻疹病毒感染期间病毒特异性IgG亚类反应的数据有限。目的:本研究的目的是基于病毒特异性IgG亚类(g1和g3)分析麻疹病毒感染。研究设计:回顾性检测三组患者的冷冻储存、血清和/或脑脊液样本;组1为麻疹原发感染14例,组2为再感染/疫苗接种失败10例,组3为亚急性硬化性全脑炎7例。方法采用改良的酶联免疫吸附试验(ELISA),采用小鼠单克隆抗体(克隆HP6091检测IgG 1,克隆HP6050检测IgG 3)。选择样品采用8 M尿素变性法检测各亚类IgG的亲和力。结果:1组患者出疹后7天内血清中IgG 3的检出率高于IgG 1。在2组病例中,在非常急性期血清样本中检测到这两种亚型。在这些病例中,IgG 1的特异性贪婪度始终高于IgG 3。在第3组中,脑脊液中检测到的igg亚类的贪婪度低于血清中的贪婪度。结论:我们的研究结果提示,在麻疹病毒感染中,与其他病毒感染一样,IgG 3应答通常发生在IgG 1应答之前,并且在初次感染时的急性期免疫中起主要作用,而IgG 1在维持免疫中起主要作用。亚急性硬化性全脑炎患者中枢神经系统中持续产生的IgG 1和IgG 3可能来源于不同于血液中的细胞群。
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