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猪胰岛素在体外对人T淋巴细胞的趋化活性。

Chemotactic activity of porcine insulin for human T lymphocytes in vitro.

作者信息

Berman J S, Center D M

出版信息

J Immunol. 1987 Apr 1;138(7):2100-3.

PMID:3549897
Abstract

T lymphocytes bear insulin receptors only after activation and entry into the cell cycle. To determine whether cell motility is concomitant with growth factor action in T lymphocytes, we measured the chemotactic activity of porcine insulin (10(-11) to 10(-5) M) for T lymphocytes. We found that the chemotactic response of human T cells activated with phytohemagglutinin (PHA) to porcine insulin was increased over that of resting T cells, with a concomitant two log leftward shift in the dose response. CD4+ and CD8+ subsets responded identically. Checkerboard analysis showed insulin to be chemotactic, as well as chemokinetic. The nature and time course of acquisition of the dose-response shift suggest that chemotaxis may be signaled by insulin acting on high affinity insulin receptors. The chemotactic effect of insulin exemplifies the general chemotactic effect of growth factors for motile target cells, and may be a useful model for the study of chemotactic signaling in T lymphocytes.

摘要

T淋巴细胞仅在激活并进入细胞周期后才携带胰岛素受体。为了确定细胞运动性是否与T淋巴细胞中生长因子的作用相伴发生,我们测量了猪胰岛素(10^(-11)至10^(-5)M)对T淋巴细胞的趋化活性。我们发现,用植物血凝素(PHA)激活的人T细胞对猪胰岛素的趋化反应比静息T细胞增强,同时剂量反应向左有两个对数级的偏移。CD4+和CD8+亚群的反应相同。棋盘分析表明胰岛素具有趋化性以及化学促动性。剂量反应偏移的性质和时间进程表明,趋化作用可能是由胰岛素作用于高亲和力胰岛素受体发出信号的。胰岛素的趋化作用例证了生长因子对运动性靶细胞的一般趋化作用,并且可能是研究T淋巴细胞趋化信号传导的有用模型。

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