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胸腺白血病抗原的非经典行为:一种非经典I类分子不依赖肽转运体的表达

Nonclassical behavior of the thymus leukemia antigen: peptide transporter-independent expression of a nonclassical class I molecule.

作者信息

Holcombe H R, Castaño A R, Cheroutre H, Teitell M, Maher J K, Peterson P A, Kronenberg M

机构信息

Department of Microbiology & Immunology, University of California, Los Angeles School of Medicine 90024, USA.

出版信息

J Exp Med. 1995 Apr 1;181(4):1433-43. doi: 10.1084/jem.181.4.1433.

Abstract

The thymus leukemia (TL) antigen is a major histocompatibility complex-encoded nonclassical class I molecule. Here we present data demonstrating that expression of the TL antigen, unlike other class I molecules, is completely independent of the function of the transporter associated with antigen processing (TAP). The TL antigen is expressed by transfected TAP-2-deficient RMA-S cells when these cells are grown at 37 degrees C. In transfected RMA cells, the kinetics of arrival of TL antigen on the cell surface are similar to those of a classical class I molecule. The kinetics are not altered in TAP-deficient RMA-S cells, demonstrating that surface TL expression in TAP-deficient cells is not due to the stable expression of a few molecules that leak out by a TAP-independent pathway. Soluble TL molecules produced by Drosophila melanogaster cells are highly resistant to thermal denaturation, unlike peptide-free classical class I molecules synthesized by these insect cells. In addition, these soluble TL molecules are devoid of detectable bound peptides. The results demonstrate that the TL antigen is capable of reaching the surface without bound peptide, although acquisition of peptide or some other ligand through a TAP-independent pathway cannot be formally excluded. We speculate that the ability of the TL antigen to reach the cell surface, under conditions in which other class I molecules do not, may be related to a specialized function of the TL molecule in the mucosal immune system, and possibly in the stimulation of intestinal gamma delta T cells.

摘要

胸腺白血病(TL)抗原是一种主要组织相容性复合体编码的非经典I类分子。在此,我们展示的数据表明,与其他I类分子不同,TL抗原的表达完全独立于与抗原加工相关的转运体(TAP)的功能。当转染的TAP - 2缺陷型RMA - S细胞在37℃培养时,它们会表达TL抗原。在转染的RMA细胞中,TL抗原到达细胞表面的动力学与经典I类分子相似。在TAP缺陷型RMA - S细胞中,动力学没有改变,这表明TAP缺陷细胞中TL抗原的表面表达并非由于少数通过不依赖TAP的途径泄漏出来的分子的稳定表达。与这些昆虫细胞合成的无肽经典I类分子不同,果蝇细胞产生的可溶性TL分子对热变性具有高度抗性。此外,这些可溶性TL分子没有可检测到的结合肽。结果表明,TL抗原能够在没有结合肽的情况下到达细胞表面,尽管通过不依赖TAP的途径获取肽或其他一些配体的可能性不能完全排除。我们推测,在其他I类分子无法到达细胞表面的条件下,TL抗原到达细胞表面的能力可能与TL分子在黏膜免疫系统中的特殊功能有关,可能还与刺激肠道γδT细胞有关。

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