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未成熟胸腺细胞抗原-1:一种区分预选和后选胸腺细胞的新型胸腺细胞标志物。

Immature thymocyte antigen-1: a novel thymocyte marker discriminating pre- and post-selected thymocytes.

作者信息

Kishi H, Tong J J, Nagata T, Muraguchi A

机构信息

Department of Immunology, Faculty of Medicine, Toyama Medical and Pharmaceutical University, Sugitani, Japan.

出版信息

Int Immunol. 1998 Jul;10(7):951-60. doi: 10.1093/intimm/10.7.951.

Abstract

Previously, we described a mAb (1-23) reacting with a novel cell surface antigen expressed on thymocytes at late CD4-CD8- [(double negative (DN)] to early CD4+CD8+ [(double positive (DP)] differentiation stage. Since the expression of this molecule was restricted to immature thymocytes, we designated it as immature thymocyte antigen-1 (IMT-1). In this study, we have investigated the relevance of IMT-1 expression to thymocyte selection using TCR transgenic mice, scid mice or RAG-2-/- mice. The IMT-1+ population in DP thymocytes was decreased in the thymuses of MHC class I-restricted or class II-restricted TCR transgenic mice with a positively selecting MHC background when compared with that of the mice with a non-selecting MHC background. IMT-1+ DP thymocytes were also decreased in TCR transgenic mice in which negative selection occurs. When DP thymocytes in H-Y TCR transgenic mice were stimulated with CD3epsilon mAb in vitro as well as in vivo, the expression of IMT-1 on DP thymocytes was decreased. Furthermore, the expression of IMT-1 on DN thymocytes from RAG-2-/- mice was drastically reduced when CD3epsilon mAb was challenged in vivo. These results suggest that the expression of IMT-1 on DP or DN thymocytes is down-regulated by stimulation through TCR as well as pre-TCR. Taken together, these results show that IMT-1 is a unique surface marker which exquisitely separates pre-selected thymocytes from post-selected thymocytes.

摘要

此前,我们描述了一种单克隆抗体(1-23),它可与一种新型细胞表面抗原发生反应,该抗原在胸腺细胞从晚期CD4-CD8- [双阴性(DN)] 向早期CD4+CD8+ [双阳性(DP)] 分化阶段表达。由于该分子的表达仅限于未成熟胸腺细胞,我们将其命名为未成熟胸腺细胞抗原-1(IMT-1)。在本研究中,我们使用TCR转基因小鼠、scid小鼠或RAG-2-/-小鼠研究了IMT-1表达与胸腺细胞选择的相关性。与具有非选择MHC背景的小鼠相比,在具有阳性选择MHC背景的MHC I类限制或II类限制TCR转基因小鼠的胸腺中,DP胸腺细胞中的IMT-1+群体减少。在发生阴性选择的TCR转基因小鼠中,IMT-1+ DP胸腺细胞也减少。当H-Y TCR转基因小鼠中的DP胸腺细胞在体外和体内用CD3ε单克隆抗体刺激时,DP胸腺细胞上IMT-1的表达降低。此外,当在体内用CD3ε单克隆抗体攻击时,RAG-2-/-小鼠的DN胸腺细胞上IMT-1的表达急剧降低。这些结果表明,通过TCR以及前TCR的刺激可下调DP或DN胸腺细胞上IMT-1的表达。综上所述,这些结果表明IMT-1是一种独特的表面标志物,可将预选胸腺细胞与后选胸腺细胞精确区分开来。

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