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首页> 外文期刊>Infection and immunity >Infection of rabbit Peyer's patches by Shigella flexneri: effect of adhesive or invasive bacterial phenotypes on follicle-associated epithelium.
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Infection of rabbit Peyer's patches by Shigella flexneri: effect of adhesive or invasive bacterial phenotypes on follicle-associated epithelium.

机译:弗氏志贺氏菌感染兔Peyer斑块:黏附或侵入性细菌表型对卵泡相关上皮细胞的影响。

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摘要

In order to invade the colonic mucosa, the bacterial pathogen Shigella flexneri must find a site of entry. Experiments with the rabbit ligated intestinal loop model described here confirm that M cells of the follicle-associated epithelium (FAE) that covers lymphoid structures of the Peyer's patches represent a major site of entry for invasive microorganisms. In addition, in an isogenic Shigella background, expression of an adhesive phenotype, or of an invasive phenotype, is required for bacteria to efficiently colonize the FAE. A nonadhesive, noninvasive mutant barely interacted with FAE. Adhesive and invasive strains induced dramatic but different alterations on FAE. Invasive strain M90T caused major inflammation-mediated tissue destruction after 8 h of infection. Adhesive strain BS15 caused limited inflammation, but major architectural changes, characterized by an increase in the size of M cells that became stretched over large pockets containing an increased number of mononuclear cells, were observed. M cells progressively occupied large surface areas of the FAE at the expense of enterocytes. This contributed to enterocytes losing contact with the lumen. These experiments demonstrate that various remodeling patterns may occur in Peyer's patches in response to bacterial pathogens, depending on the virulence phenotype expressed by the pathogenic strain.
机译:为了侵入结肠粘膜,细菌病原菌志贺氏菌必须找到进入位点。此处描述的兔结扎肠环模型的实验证实,覆盖Peyer斑淋巴结构的卵泡相关上皮(FAE)的M细胞代表了侵入性微生物的主要进入部位。另外,在等基因志贺氏菌背景中,细菌要有效地定殖于FAE,需要表达粘附性表型或侵入性表型。一个非粘附性,非侵入性突变体几乎与FAE相互作用。粘附性和侵入性菌株在FAE上引起了巨大但不同的变化。感染8小时后,侵袭性菌株M90T引起了主要的炎症介导的组织破坏。粘附菌株BS15引起有限的炎症,但是观察到主要的结构变化,其特征在于M细胞的尺寸增加,该M细胞的尺寸变得更大,该M细胞的尺寸被拉伸到包含增加数量的单核细胞的大口袋上。 M细胞逐渐消耗FAE的大表面积,而以肠上皮细胞为代价。这导致肠细胞失去与管腔的接触。这些实验表明,取决于细菌病原体表达的毒力表型,响应细菌病原体,Peyer斑块中可能会发生各种重塑模式。

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