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血吸虫免疫:疫苗研发进展

Immunity to schistosomes: progress toward vaccine.

作者信息

Capron A, Dessaint J P, Capron M, Ouma J H, Butterworth A E

机构信息

Centre d'Immunologie et de Biologie Parasitaire, Unité Mixte INSERM 167-CNRS 624, Institut Pasteur, Lille, France.

出版信息

Science. 1987 Nov 20;238(4830):1065-72. doi: 10.1126/science.3317823.

Abstract

Among the major parasitic infections, schistosomiasis may be the most promising candidate for human vaccination. Information about mechanisms of immunity, gained mainly from experimental models but likely to be relevant to human infection, indicates a dynamic balance between protective and regulatory (blocking) mechanisms. Besides cell-mediated responses leading to macrophage activation, antibody-dependent cell-mediated cytotoxicity systems involving precise antibody isotypes and nonlymphoid cells (mononuclear phagocytes, eosinophils, and platelets) appear to be essential effectors of immune attack. The slow development of immunity in humans seems related to the production of antibodies that cross-react with schistosomulum surface antigen and block the binding of antibodies of the effector isotype. Schistosomes that survive in the bloodstream and produce chronic infections may evade the immune system as a result of intrinsic changes in membrane susceptibility and of transient expression of target antigens; at other stages of the parasite life cycle, cross-reactive molecules may be secreted that play an essential role in the induction of immunity. Several schistosome proteins have been characterized as candidates for vaccination. Among these, an antigen of 28 kilodaltons has been cloned and shown to be immunogenic in humans and protective in mice, rats, and baboons.

摘要

在主要的寄生虫感染中,血吸虫病可能是人类疫苗接种最有前景的候选对象。关于免疫机制的信息,主要来自实验模型但可能与人类感染相关,表明在保护性和调节性(阻断性)机制之间存在动态平衡。除了导致巨噬细胞活化的细胞介导反应外,涉及精确抗体亚型和非淋巴细胞(单核吞噬细胞、嗜酸性粒细胞和血小板)的抗体依赖性细胞介导细胞毒性系统似乎是免疫攻击的重要效应器。人类免疫的缓慢发展似乎与产生与童虫表面抗原交叉反应并阻断效应器亚型抗体结合的抗体有关。在血液中存活并产生慢性感染的血吸虫可能由于膜敏感性的内在变化和靶抗原的瞬时表达而逃避免疫系统;在寄生虫生命周期的其他阶段,可能会分泌交叉反应分子,这些分子在免疫诱导中起重要作用。几种血吸虫蛋白已被鉴定为疫苗接种的候选对象。其中,一种28千道尔顿的抗原已被克隆,并显示在人类中具有免疫原性,在小鼠、大鼠和狒狒中具有保护性。

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