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曼氏血吸虫培养童虫和成虫表面的补体调节

Complement regulation on the surface of cultured schistosomula and adult worms of Schistosoma mansoni.

作者信息

Marikovsky M, Parizade M, Arnon R, Fishelson Z

机构信息

Department of Chemical Immunology, Weizmann Institute of Science, Rehovot, Israel.

出版信息

Eur J Immunol. 1990 Jan;20(1):221-7. doi: 10.1002/eji.1830200132.

Abstract

Cercaria and freshly prepared schistosomula of Schistosoma mansoni are highly sensitive to complement. However, early in their maturation, the schistosomula become resistant to complement killing. This conversion is preceded by a rapid and massive release of several acetabular proteases and of the glycocalyx coat. Thus, shedding of the glycocalyx which is a major immunogen and a strong activator of the alternative pathway of complement permits the parasite to escape immune damage. Mechanically transformed schistosomula, which were cultured in a defined synthetic medium and developed complement resistance, could be converted by proteolysis to complement sensitivity. Trypsin and pronase markedly increased the susceptibility of cultured schistosomula to complement. The trypsin-induced complement sensitivity persisted for at least 19 h without recovery of resistance. Similar treatment with trypsin produced complete killing of adult worms by complement in absence of antibodies. Efficient killing was obtained with normal human serum (NHS), with normal guinea pig serum (GpS), and with C4-depleted HS and C4-deficient GpS indicating that the killing was mediated by the cytolytic alternative pathway of complement. Larger quantities of C3b with intact alpha' chain could be demonstrated on trypsin-treated than on non-treated schistosomula. Antibodies which were raised in rabbits by immunization with the trypsin-released material bound to cultured (non-treated) schistosomula and to adult worms, and induced their killing in GpS and C4-deficient GpS. These results suggest that following release of the glycocalyx, the transforming schistosomula of S. mansoni spontaneously express a complement regulatory protein(s). A similar regulator is postulated to be present on the surface of adult worms. Such regulatory molecules may serve as good targets for immunotherapy, since antibodies directed to them will inhibit their regulatory activity and thus potentiate in vivo the lytic action of complement.

摘要

曼氏血吸虫的尾蚴和新制备的童虫对补体高度敏感。然而,在其成熟早期,童虫会对补体杀伤产生抗性。这种转变之前会快速大量释放几种吸盘蛋白酶和糖萼层。因此,作为主要免疫原和补体替代途径强激活剂的糖萼层的脱落,使寄生虫能够逃避免疫损伤。在特定合成培养基中培养并产生补体抗性的机械转化童虫,可通过蛋白水解作用转化为对补体敏感。胰蛋白酶和链霉蛋白酶显著增加了培养的童虫对补体的敏感性。胰蛋白酶诱导的补体敏感性至少持续19小时,抗性未恢复。在没有抗体的情况下,用胰蛋白酶进行类似处理可使成虫被补体完全杀死。用人正常血清(NHS)、豚鼠正常血清(GpS)以及C4缺失的人血清和C4缺陷的豚鼠血清都能实现高效杀伤,这表明杀伤是由补体的溶细胞替代途径介导的。与未处理的童虫相比,在经胰蛋白酶处理的童虫上可检测到更多具有完整α'链的C3b。用胰蛋白酶释放的物质免疫家兔产生的抗体,能与培养的(未处理的)童虫及成虫结合,并在GpS和C4缺陷的GpS中诱导它们被杀伤。这些结果表明,在糖萼层释放后,曼氏血吸虫正在转化的童虫会自发表达一种补体调节蛋白。推测成虫表面也存在类似的调节因子。这种调节分子可能是免疫治疗的良好靶点,因为针对它们的抗体将抑制其调节活性,从而在体内增强补体的溶解作用。

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