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副溶血性弧菌耐热直接溶血素调节肠道培养细胞中的细胞骨架组织和钙稳态。

Vibrio parahaemolyticus thermostable direct hemolysin modulates cytoskeletal organization and calcium homeostasis in intestinal cultured cells.

作者信息

Fabbri A, Falzano L, Frank C, Donelli G, Matarrese P, Raimondi F, Fasano A, Fiorentini C

机构信息

Department of Ultrastructures, Istituto Superiore di Sanità, Rome, Italy.

出版信息

Infect Immun. 1999 Mar;67(3):1139-48. doi: 10.1128/IAI.67.3.1139-1148.1999.

Abstract

Vibrio parahaemolyticus is a marine bacterium known to be the leading cause of seafood gastroenteritis worldwide. A 46-kDa homodimer protein secreted by this microorganism, the thermostable direct hemolysin (TDH), is considered a major virulence factor involved in bacterial pathogenesis since a high percentage of strains of clinical origin are positive for TDH production. TDH is a pore-forming toxin, and its most extensively studied effect is the ability to cause hemolysis of erythrocytes from different mammalian species. Moreover, TDH induces in a variety of cells cytotoxic effects consisting mainly of cell degeneration which often leads to loss of viability. In this work, we examined the cellular changes induced by TDH in monolayers of IEC-6 cells (derived from the rat crypt small intestine), which represent a useful cell model for studying toxins from enteric bacteria. In experimental conditions allowing cell survival, TDH induces a rapid transient increase in intracellular calcium as well as a significant though reversible decreased rate of progression through the cell cycle. The morphological changes seem to be dependent on the organization of the microtubular network, which appears to be the preferential cytoskeletal element involved in the cellular response to the toxin.

摘要

副溶血性弧菌是一种海洋细菌,已知是全球海鲜肠胃炎的主要病因。这种微生物分泌的一种46千道尔顿的同型二聚体蛋白,即耐热直接溶血素(TDH),被认为是参与细菌致病机制的主要毒力因子,因为临床来源的菌株中有很高比例的TDH产生呈阳性。TDH是一种成孔毒素,其研究最广泛的作用是能够导致不同哺乳动物物种的红细胞溶血。此外,TDH在多种细胞中诱导细胞毒性作用,主要包括细胞变性,这常常导致细胞活力丧失。在这项研究中,我们检测了TDH在IEC-6细胞(源自大鼠隐窝小肠)单层中诱导的细胞变化,IEC-6细胞是研究肠道细菌毒素的有用细胞模型。在允许细胞存活的实验条件下,TDH诱导细胞内钙迅速短暂增加,以及细胞周期进程速率显著但可逆的下降。形态学变化似乎取决于微管网络的组织,微管网络似乎是参与细胞对毒素反应的优先细胞骨架成分。

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