淋巴因子激活的人单核细胞的细胞抑制和吞噬能力。

G Unsgaard
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引用次数: 0

摘要

通过暴露于bcg刺激淋巴细胞的淋巴因子上清液(LS),人单核细胞对人细胞系NHIK 3025具有细胞抑制作用。暴露于LS 1,2,4小时诱导单核细胞具有相当大的细胞抑制能力。然而,暴露于LS 24小时和72小时后,具有更强的细胞抑制作用。将LS激活的单核细胞对125i标记的白色念珠菌的吞噬作用与对照上清(CS)处理的单核细胞的吞噬作用进行比较。短时间暴露于LS会增加摄取量。然而,暴露于LS 72小时会导致摄取能力下降。ls激活的单核细胞消化摄入的白色念珠菌的能力受到抑制。ls激活的单核细胞DNA合成增加,而蛋白质合成无明显影响。LS激活的单核细胞在去除LS后培养24小时,细胞抑制能力消失。在去除LS或CS并进行后续培养4天后,LS处理的细胞分化的形态和功能迹象比CS处理的细胞更不明显。前者细胞的存活率也降低了。然而,这些细胞在再次暴露于LS后被强烈地重新激活。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Cytostatic and phagocytic capacity of lymphokine-activated human monocytes.

Human monocytes were rendered cytostatic to the human cell line NHIK 3025 by exposure to lymphokine supernatants (LS) from BCG-stimulated lymphocytes. Exposure to LS for 1, 2 and 4 h induced a considerable cytostatic capacity in the monocytes. However, a stronger cytostatic effect was acquired by exposure to LS for 24 h and 72 h. The phagocytosis of 125I-labelled Candida albicans by LS-activated monocytes was compared with phagocytosis by monocytes treated with control supernatants (CS). The ingestion was increased by short exposure to LS. However, a 72-h exposure to LS induced a decreased ingestion capacity. The capacity of the LS-activated monocytes to digest ingested C. albicans was suppressed. DNA synthesis was increased in the LS-activated monocytes, while protein synthesis was not significantly influenced. The cytostatic capacity of LS-activated monocytes was abolished by culture for 24 h after removal of LS. Following removal of LS or CS with subsequent culture for 4 days, morphological and functional signs of differentiation were less marked in the LS-treated than in the CS-treated cells. The survival was also reduced in the former cells. However, these cells were strongly reactivated by re-exposure to LS.

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