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TAP对肽受体性主要组织相容性复合体I类分子的产生及细胞内运输的影响

Effect of TAP on the generation and intracellular trafficking of peptide-receptive major histocompatibility complex class I molecules.

作者信息

Day P M, Esquivel F, Lukszo J, Bennink J R, Yewdell J W

机构信息

Laboratory of Viral Diseases, National Institute of Allergy and Infectious Diseases, Bethesda, Maryland 20892.

出版信息

Immunity. 1995 Feb;2(2):137-47. doi: 10.1016/s1074-7613(95)80014-x.

Abstract

Using a fluorescein-conjugated antigenic peptide, peptide-receptive H-2Kb MHC class I molecules were found throughout the secretory pathways of RMA cells and peptide transporter (TAP)-deficient derivative cells (RMA/S). RMA/S cells displayed higher levels of intracellular peptide-receptive molecules, while, surprisingly, RMA cells expressed 3- to 5-fold more cell surface peptide-receptive molecules. Metabolic radiolabeling of Kb-associated oligosaccharides with [1-3H]galactose demonstrated that despite a large difference in the fraction of Kb molecules in native conformation in detergent extracts, Kb transport rates from the trans-Golgi complex to the surfaces of RMA and RMA/S cells were similar. Thus, although considerable numbers of class I alpha chains reach the RMA/S cell surface, they are a less productive source of peptide-receptive molecules than class I molecules synthesized by TAP-expressing RMA cells, suggesting paradoxically that TAP functions to increase the amount of peptide-receptive molecules at the cell surface.

摘要

利用一种荧光素偶联的抗原肽,在RMA细胞和肽转运体(TAP)缺陷的衍生细胞(RMA/S)的整个分泌途径中都发现了肽反应性H-2Kb I类主要组织相容性复合体分子。RMA/S细胞表现出更高水平的细胞内肽反应性分子,而令人惊讶的是,RMA细胞表达的细胞表面肽反应性分子多3至5倍。用[1-³H]半乳糖对与Kb相关的寡糖进行代谢性放射性标记表明,尽管在去污剂提取物中天然构象的Kb分子比例存在很大差异,但从反式高尔基体复合体到RMA和RMA/S细胞表面的Kb转运速率相似。因此,尽管相当数量的I类α链到达RMA/S细胞表面,但与表达TAP的RMA细胞合成的I类分子相比,它们作为肽反应性分子的来源效率较低,这看似矛盾地表明TAP的作用是增加细胞表面肽反应性分子的数量。

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