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分枝杆菌对巨噬细胞辅助细胞活性的调节。I. 感染微小分枝杆菌的正常和辐照小鼠中Ia抗原的表达

Regulation of macrophage accessory cell activity by mycobacteria. I. Ia expression in normal and irradiated mice infected with Mycobacterium microti.

作者信息

Kaye P M, Feldmann M

出版信息

Clin Exp Immunol. 1986 Apr;64(1):20-7.

Abstract

CBA/Ca mice were infected by either the intravenous or intraperitoneal route with Mycobacterium microti and the subsequent changes in local macrophage populations examined. Following infection, the number of macrophages increased and they showed greater expression of both MHC Class II molecules. This response was not dependent on viability of the mycobacteria, in contrast to reports with other microorganisms such as Listeria. Studies in sublethally irradiated mice indicated that persistent antigen could give rise to a response after a period of host recovery which was radiation dose dependent. This procedure also highlighted differences in the regulation of different murine class II antigens in vivo, as seen by delayed re-expression of I-E antigens. Macrophage accessory cell function, as assessed by an in vitro T cell proliferation assay, correlated with Ia expression after fixation, but not after indomethacin treatment; this highlights the diverse nature of regulatory molecules produced by these cells.

摘要

通过静脉内或腹腔内途径用微小分枝杆菌感染CBA/Ca小鼠,并检测局部巨噬细胞群体随后的变化。感染后,巨噬细胞数量增加,并且它们显示出MHC II类分子的表达增加。与其他微生物(如李斯特菌)的报道相反,这种反应不依赖于分枝杆菌的活力。对亚致死剂量照射小鼠的研究表明,持续存在的抗原在宿主恢复一段时间后可引发反应,且该反应依赖于辐射剂量。该过程还突出了体内不同小鼠II类抗原调节的差异,如I-E抗原延迟重新表达所见。通过体外T细胞增殖试验评估的巨噬细胞辅助细胞功能,与固定后的Ia表达相关,但与吲哚美辛处理后的表达无关;这突出了这些细胞产生的调节分子的多样性。

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