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人白细胞介素-2受体α链转基因小鼠中白细胞介素-2诱导的增殖反应所揭示的小鼠白细胞介素-2受体β链在胸腺和脾淋巴细胞亚群上的表达。

Expression of murine IL-2 receptor beta-chain on thymic and splenic lymphocyte subpopulations as revealed by the IL-2-induced proliferative response in human IL-2 receptor alpha-chain transgenic mice.

作者信息

Hattori M, Okazaki H, Ishida Y, Onuma M, Kano S, Honjo T, Minato N

机构信息

Department of Veterinary Medicine, Hokkaido University, Sapporo, Japan.

出版信息

J Immunol. 1990 May 15;144(10):3809-15.

PMID:2332632
Abstract

Lymphocytes from the human (h) IL-2R alpha chain transgenic mice (TGM) constitutively express high affinity binding sites for hIL-2, consisting of transgenic h-IL-2R alpha and endogenous murine IL-2R beta, and therefore easily proliferate in vitro in response to hIL-2. Our study was undertaken to clarify the hIL-2-responsive lymphocyte subsets in the TGM, which should most likely reflect the normal distribution of m IL-2R beta expression. In both thymus and spleen, the majority of expanded cells by hIL-2 was CD3+CD4-CD8+ TCR alpha beta+ cells. The proliferation of CD4+ cells was not observed at all from either organ despite the expression of transgenic hIL-2R alpha. Potent cellular proliferation was also observed from the thymocytes that had been depleted of CD8+ cells, the expanded cells consisting of CD3- (15-40%) and CD3+ populations (60-85%). Among CD3+ cells, approximately the half portion expressed TCR alpha beta, whereas the other half was suggested to express TCR gamma delta. A variable portion (5-20%) of the CD3+ cells expressed CD8 (Lyt-2) in the absence of Lyt-3, and the CD3+CD8+ cells were confined preferentially to the TCR alpha beta- (TCR gamma delta+) population. In the culture of splenocytes depleted of CD8+ cells, however, the proliferated cells were mostly CD3-CD4-CD8-TCR-Mac1-, whereas a minor portion (10-30%) was CD3+CD4-CD8-TCR alpha beta- (TCR gamma delta+. Analysis of TCR genes at both DNA and mRNA levels confirmed the phenotypical observations. These results strongly suggested that IL-2R beta was constitutively and selectively expressed on the primary murine thymocytes and splenic T and NK cells, except for CD4+ cells in both organs.

摘要

来自人(h)白细胞介素-2受体α链转基因小鼠(TGM)的淋巴细胞组成性表达对hIL-2的高亲和力结合位点,该位点由转基因h-IL-2Rα和内源性鼠IL-2Rβ组成,因此在体外易因hIL-2而增殖。我们开展本研究以阐明TGM中对hIL-2有反应的淋巴细胞亚群,这很可能反映了鼠IL-2Rβ表达的正常分布。在胸腺和脾脏中,经hIL-2扩增的大多数细胞是CD3 + CD4 - CD8 + TCRαβ +细胞。尽管有转基因hIL-2Rα的表达,但在这两个器官中均未观察到CD4 +细胞的增殖。从已去除CD8 +细胞的胸腺细胞中也观察到了强劲的细胞增殖,扩增的细胞由CD3 -(15 - 40%)和CD3 +群体(60 - 85%)组成。在CD3 +细胞中,大约一半表达TCRαβ,而另一半则提示表达TCRγδ。在不存在Lyt-3的情况下,可变比例(5 - 20%)的CD3 +细胞表达CD8(Lyt-2),并且CD3 + CD8 +细胞优先局限于TCRαβ -(TCRγδ +)群体。然而,在去除CD8 +细胞的脾细胞培养物中,增殖的细胞大多是CD3 - CD4 - CD8 - TCR - Mac1 -,而一小部分(10 - 30%)是CD3 + CD4 - CD8 - TCRαβ -(TCRγδ +)。在DNA和mRNA水平对TCR基因的分析证实了表型观察结果。这些结果强烈表明,IL-2Rβ在原代鼠胸腺细胞以及脾脏T细胞和NK细胞上组成性且选择性地表达,但两个器官中的CD4 +细胞除外。

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