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在人T淋巴细胞亚群中,CD45R0+细胞中CD3抗原介导的钙信号和蛋白激酶C激活作用比CD45RA+细胞中的更强。

CD3 antigen-mediated calcium signals and protein kinase C activation are higher in CD45R0+ than in CD45RA+ human T lymphocyte subsets.

作者信息

Robinson A T, Miller N, Alexander D R

机构信息

Department of Immunology, Institute of Animal Physiology & Genetics Research, Babraham, Cambridge.

出版信息

Eur J Immunol. 1993 Jan;23(1):61-8. doi: 10.1002/eji.1830230111.

Abstract

T lymphocytes may be separated into subsets according to their expression of CD45 isoforms. The CD45R0+ T cell subset has been reported to proliferate in response to recall antigen and to mitogenic mAb to a much greater extent than the CD45RA+ subset. This difference could be due to more efficient coupling of the T cell antigen receptor complex to mitogenic signaling pathways. To investigate this possibility, CD3 antigen-induced calcium signals, diacylglycerol (DAG) production and protein kinase C (PKC) activation levels were compared in CD45RA+ and CD45R0+ human T lymphocyte subsets derived from peripheral blood. The mean CD3-induced rise in intracellular calcium was 80% greater in CD45R0+ than in CD45RA+ cells. Basal DAG levels in CD45R0+ cells were found to be, on average, 60% higher than in CD45RA+ cells (p = 0.002), but the CD3-induced production of DAG over background was not different in the two subsets (p = 0.4). Basal PKC activity, and CD3-induced PKC activation levels over background, were found to be 50% and 140% higher, respectively, in CD45R0+ cells than in CD45RA+ cells (p = 0.015 and 0.023). The CD45R0+ subset contained a higher proportion of cells expressing activation markers, such as CD25, CD71 and major histocompatibility complex class II, when compared to the CD45RA+ subset. Our results suggest that the elevated basal DAG levels observed in the CD45R0+ subset may reflect the recent activation of these cells. Both the higher basal DAG and CD3-induced elevation in intracellular calcium observed in the CD45R0+ cells may contribute to the greater PKC activation signals triggered by CD3 mAb in this subset. These findings elucidate the greater response of CD45R0+ T cells to mitogenic stimuli compared to CD45RA+ cells.

摘要

T淋巴细胞可根据其CD45异构体的表达分为不同亚群。据报道,CD45R0 + T细胞亚群对回忆抗原和促有丝分裂单克隆抗体的增殖反应比CD45RA +亚群大得多。这种差异可能是由于T细胞抗原受体复合物与促有丝分裂信号通路的偶联更有效。为了研究这种可能性,我们比较了来自外周血的CD45RA +和CD45R0 +人T淋巴细胞亚群中CD3抗原诱导的钙信号、二酰基甘油(DAG)产生和蛋白激酶C(PKC)激活水平。CD45R0 +细胞中CD3诱导的细胞内钙平均升高幅度比CD45RA +细胞大80%。发现CD45R0 +细胞中的基础DAG水平平均比CD45RA +细胞高60%(p = 0.002),但两个亚群中CD3诱导的DAG产生量超过背景值的情况没有差异(p = 0.4)。发现CD45R0 +细胞中的基础PKC活性以及CD3诱导的PKC激活水平超过背景值的幅度分别比CD45RA +细胞高50%和140%(p = 0.015和0.023)。与CD45RA +亚群相比,CD45R0 +亚群中表达激活标志物(如CD25、CD71和主要组织相容性复合体II类)的细胞比例更高。我们的结果表明,在CD45R0 +亚群中观察到的基础DAG水平升高可能反映了这些细胞最近的激活状态。在CD45R0 +细胞中观察到的基础DAG水平升高和CD3诱导的细胞内钙升高都可能导致该亚群中CD3单克隆抗体触发的更大的PKC激活信号。这些发现阐明了CD45R0 + T细胞与CD45RA +细胞相比对促有丝分裂刺激的更大反应。

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