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克氏锥虫感染增强了人类恰加斯病急性病例中的多反应性抗体反应。

Trypanosoma cruzi infection enhances polyreactive antibody response in an acute case of human Chagas' disease.

作者信息

Grauert M R, Houdayer M, Hontebeyrie-Joskowciz M

机构信息

Unité d'Immunohématologie et d'Immuno Pathologie, Institut Pasteur, Paris, France.

出版信息

Clin Exp Immunol. 1993 Jul;93(1):85-92. doi: 10.1111/j.1365-2249.1993.tb06501.x.

Abstract

The kinetics of antibody response in an acute case of human Chagas' disease was investigated. Hypergammaglubulinaemia appeared at day 17 of infection, and persisted after 66 days of infection, at which time parasitaemia became undetectable. Titration of immunoglobulins showed that the three principal isotypes were involved in the response, emphasizing polyclonal B cell activation. Total IgA was detected before total IgM, and the latter before total IgG. High titres of autoantibodies were found among IgM and IgG subclasses. IgA was also the first isotype to be detected among specific anti-Trypanosoma cruzi antibodies. However, the maximal parasite antibody response was attained after 30 days of infection for all isotypes. With regard to possible cross-reactivity between molecules of host and parasite, adsorption experiments on T. cruzi-specific immunosorbent were designed. Specific antibodies, present in the eluates, also recognized natural antigens, especially laminin. In order to characterize the alpha-galactose epitope of laminin, adsorption experiments on sheep erythrocytes were performed, and revealed the possible presence of another epitope on the glycoprotein. Our results indicate that in the case of Chagas' disease investigated here, polyclonal activation occurred; moreover, they suggest that molecular mimicry may play a role by increasing autoantibodies, probably via a parasite-driven mechanism.

摘要

对一例人类恰加斯病急性病例的抗体反应动力学进行了研究。感染第17天出现高丙种球蛋白血症,并在感染66天后持续存在,此时寄生虫血症变得无法检测到。免疫球蛋白滴定显示三种主要同种型参与了反应,强调了多克隆B细胞活化。总IgA在总IgM之前被检测到,后者在总IgG之前被检测到。在IgM和IgG亚类中发现了高滴度的自身抗体。IgA也是在特异性抗克氏锥虫抗体中首先被检测到的同种型。然而,所有同种型在感染30天后达到最大寄生虫抗体反应。关于宿主和寄生虫分子之间可能的交叉反应,设计了在克氏锥虫特异性免疫吸附剂上的吸附实验。洗脱液中存在的特异性抗体也识别天然抗原,尤其是层粘连蛋白。为了表征层粘连蛋白的α-半乳糖表位,进行了在绵羊红细胞上的吸附实验,并揭示了糖蛋白上可能存在另一种表位。我们的结果表明,在此研究的恰加斯病病例中发生了多克隆活化;此外,它们表明分子模拟可能通过增加自身抗体发挥作用,可能是通过寄生虫驱动的机制。

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本文引用的文献

1
THE NATURAL-SELECTION THEORY OF ANTIBODY FORMATION.抗体形成的自然选择理论。
Proc Natl Acad Sci U S A. 1955 Nov 15;41(11):849-57. doi: 10.1073/pnas.41.11.849.

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