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克氏锥虫亚群对巨噬细胞激活和调理抗体的诱导作用。

Induction of macrophage activation and opsonizing antibodies by Trypanosoma cruzi subpopulations.

作者信息

Celentano A M, González Cappa S M

机构信息

Department of Microbiology, Faculty of Medicine, University of Buenos Aires, Argentina.

出版信息

Parasite Immunol. 1992 Mar;14(2):155-67. doi: 10.1111/j.1365-3024.1992.tb00458.x.

Abstract

Macrophage activation and production of opsonizing antibodies were studied in mice either infected with a lethal and reticulotropic Trypanosoma cruzi strain, RA, or with a non lethal and myotropic strain, CA-I, as well as with a clone, K98 (derived from CA-I), similar to the parental strain. Measurement of macrophage respiratory burst by chemiluminescence disclosed that T. cruzi infection induced an enhancement of the respiratory burst, no matter the parasite subpopulation employed. But, while in mice surviving RA infection the respiratory burst was higher than during the acute period and parasitaemia was efficiently controlled, in mice infected with K98 enhanced respiratory burst coexisted with measurable levels of parasitaemia either at acute or chronic infection periods. Macrophage activation was also proved by enhanced trypanocidal activity in macrophages derived from mice infected with any of the parasite subpopulations. Sera from RA mice opsonized and lysed T. cruzi bloodstream forms efficiently, whereas sera from CA-I or K98 mice neither lysed nor opsonized this parasite stage. All three subpopulations assayed here showed IgG bound to their membranes in vivo and similar capping kinetics, but only antibodies bound to RA parasites invariably triggered lysis. Therefore, the role played by macrophage activation in resistance and control of Pm levels is related to some features of each T. cruzi subpopulation, such as its capacity to invade macrophages and to elicit opsonizing antibodies.

摘要

在感染致死性且嗜网状内皮系统的克氏锥虫菌株RA、非致死性且嗜肌的菌株CA-I以及与亲代菌株相似的克隆K98(源自CA-I)的小鼠中,研究了巨噬细胞活化和调理素抗体的产生。通过化学发光法测量巨噬细胞呼吸爆发发现,无论使用哪种寄生虫亚群,克氏锥虫感染均会诱导呼吸爆发增强。但是,在感染RA后存活的小鼠中,呼吸爆发高于急性期,且寄生虫血症得到有效控制,而在感染K98的小鼠中,无论是在急性还是慢性感染期,增强的呼吸爆发都与可测量的寄生虫血症水平并存。来自感染任何一种寄生虫亚群的小鼠的巨噬细胞中杀锥虫活性增强也证明了巨噬细胞的活化。RA小鼠的血清可有效调理并裂解克氏锥虫血流形式,而CA-I或K98小鼠的血清既不能裂解也不能调理该寄生虫阶段。此处检测的所有三个亚群在体内均显示IgG与其膜结合且具有相似的封帽动力学,但只有与RA寄生虫结合的抗体始终会引发裂解。因此,巨噬细胞活化在抵抗和控制寄生虫水平中所起的作用与每个克氏锥虫亚群的某些特征有关,例如其侵入巨噬细胞和引发调理素抗体的能力。

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