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首页> 外文期刊>Infection and immunity >Interaction of Chlamydia psittaci with mouse peritoneal macrophages.
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Interaction of Chlamydia psittaci with mouse peritoneal macrophages.

机译:鹦鹉热衣原体与小鼠腹膜巨噬细胞的相互作用。

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L-cell-grown Chlamydia psittaci elementary bodies (EB) were rapidly phagocytized by mouse peritoneal macrophages in vitro. However, the intracellular fate of chlamydiae in macrophages appeared to be dependent on the multiplicity of infection (MOI), i.e., the EB-to-macrophage ratio, and the treatment of the EB. At an MOI of 1:1 or less, survival is maximal, and growth and multiplication of live, untreated chlamydiae did occur. In contrast, at a high MOI (100:1), survival of chlamydiae is reduced, as confirmed by release of 3H-labeled nucleic acid into the supernatant. At the high MOI, macrophage damage occurred that resulted in significant release of the lactic dehydrogenase, beginning 2 h postinfection. This immediated macrophage cytotoxicity as abolished by pretreatment of EB with heat (5 min at 56 degrees C) and was reduced about 50% by coating EB with homologous antibody. Pretreatment of the chlamydia with heat or opsonizing antibody provides increased uptake of EB by macrophages but may contribute to increased destruction of these obligate intracellular pathogens in professional phagocytic cells.
机译:L细胞生长的衣原体衣原体(EB)被小鼠腹膜巨噬细胞在体外迅速吞噬。然而,巨噬细胞中衣原体的细胞内命运似乎取决于感染的复数(MOI),即,EB与巨噬细胞的比例以及EB的治疗。当MOI为1:1或更低时,存活率是最大的,并且确实发生了未经治疗的活衣原体的生长和繁殖。相反,在高MOI(100:1)时,衣原体的存活率降低,这可通过将3H标记的核酸释放到上清液中来确认。在高MOI时,发生巨噬细胞损害,导致感染后2小时开始大量释放乳酸脱氢酶。通过加热(在56摄氏度下5分钟)对EB进行预处理,可以消除这种立即的巨噬细胞毒性,并通过用同源抗体包被EB将其降低约50%。用热或调理抗体对衣原体进行预处理可增加巨噬细胞对EB的吸收,但可能有助于增加专业吞噬细胞中这些专性细胞内病原体的破坏。

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