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克氏锥虫:在哺乳动物细胞中的入侵机制及细胞内命运

Trypanosoma cruzi: mechanism of entry and intracellular fate in mammalian cells.

作者信息

Nogueira N, Cohn Z

出版信息

J Exp Med. 1976 Jun 1;143(6):1402-20. doi: 10.1084/jem.143.6.1402.

Abstract

The mode of entry and intracellular fate of epimastigotes and trypomastigotes of Trypanosoma cruzi in cultured cells was studied. Electron microscopic observations indicated the uptake by phagocytosis of both forms into mouse peritoneal macrophages and of trypomastigotes and transition forms into other cultured cell types. In each instance the organisms were initially surrounded by a plasma membrane-derived phagosome. Trypsin and chymotrypsin treatment of the macrophages completely abolished attachment and ingestion of both forms, indicating that protease-sensitive structures on the macrophage plasma membrane mediate ingestion. The macrophage Fc or C3b receptors were not essential for uptake of T. cruzi in the conditions used. Cytochalasin B inhibited ingestion but not the attachment of both forms by macrophages. Epimastigotes were not taken up by HeLa, L cells, and calf embryo fibroblasts. In macrophages, epimastigotes were killed and digested within phagolysosomes. In contrast, trypomastigotes and transition forms escaped from the phagocytic vacuole and then multiplied in the cytoplasmic matrix. Amastigotes released from infected cells exhibited properties similar to those of trypomastigotes and were able to enter all cell types studied and multiply intracellularly.

摘要

研究了克氏锥虫的上鞭毛体和锥鞭毛体在培养细胞中的进入方式和细胞内命运。电子显微镜观察表明,两种形态的虫体均通过吞噬作用被小鼠腹腔巨噬细胞摄取,锥鞭毛体和过渡型被其他培养细胞类型摄取。在每种情况下,虫体最初都被源自质膜的吞噬体包围。用胰蛋白酶和胰凝乳蛋白酶处理巨噬细胞可完全消除两种形态的附着和摄取,这表明巨噬细胞质膜上对蛋白酶敏感的结构介导摄取。在所使用的条件下,巨噬细胞的Fc或C3b受体对于克氏锥虫的摄取并非必需。细胞松弛素B抑制巨噬细胞对两种形态的摄取,但不抑制其附着。HeLa细胞、L细胞和小牛胚胎成纤维细胞不摄取上鞭毛体。在巨噬细胞中,上鞭毛体在吞噬溶酶体内被杀死并消化。相反,锥鞭毛体和过渡型从吞噬泡中逸出,然后在细胞质基质中增殖。从受感染细胞释放的无鞭毛体表现出与锥鞭毛体相似的特性,能够进入所有研究的细胞类型并在细胞内增殖。

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