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链球菌M蛋白对人血中血小板和多形核白细胞的毒性作用。

Toxic effects of streptococcal M protein on platelets and polymorphonuclear leukocytes in human blood.

作者信息

Beachey E H, Stollerman G H

出版信息

J Exp Med. 1971 Aug 1;134(2):351-65. doi: 10.1084/jem.134.2.351.

Abstract

Purified M protein isolated from Group A streptococci produced cytotoxic reactions in normal human blood in vitro. In the presence of M antigen, platelets aggregated, fused, and lysed. Polymorphonuclear leukocytes (PMN) surrounded the platelet aggregates, then became highly vacuolated and lysed. In addition, PMN progressively lost their capacity to phagocytose unrelated bacteria and to migrate in glass capillary pipettes. Platelet-PMN reactions were directly proportional to the type-specific precipitin reactivity of each M preparation and could be removed with homologous M antibody, only. Moreover, the reactivity of M protein was abolished by enzymatic digestion with trypsin, but not with lysozyme, strongly suggesting that cell-wall mucopeptide was not involved. Preliminary studies showed that platelet-PMN reactions require heat-stable and heat-labile serum factors, presumably antibody and complement. It is suggested that cytotoxic determinants are uncovered by the extraction and purification process and are intimately associated with the type-specific M determinant, possibly in a molecular complex.

摘要

从A组链球菌中分离出的纯化M蛋白在体外可使正常人血液产生细胞毒性反应。在M抗原存在的情况下,血小板聚集、融合并裂解。多形核白细胞(PMN)围绕血小板聚集体,随后出现高度空泡化并裂解。此外,PMN逐渐丧失吞噬无关细菌以及在玻璃毛细管中迁移的能力。血小板 - PMN反应与每种M制剂的型特异性沉淀素反应性成正比,并且只能用同源M抗体消除。此外,用胰蛋白酶进行酶消化可消除M蛋白的反应性,但溶菌酶则不能,这强烈表明细胞壁粘肽不参与其中。初步研究表明,血小板 - PMN反应需要热稳定和热不稳定的血清因子,推测为抗体和补体。有人提出,细胞毒性决定簇在提取和纯化过程中被暴露出来,并与型特异性M决定簇密切相关,可能存在于分子复合物中。

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