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极化的犬肾细胞中主要组织相容性复合体II类恒定链运输的结构要求

Structural requirements for major histocompatibility complex class II invariant chain trafficking in polarized Madin-Darby canine kidney cells.

作者信息

Odorizzi G, Trowbridge I S

机构信息

Department of Cancer Biology, The Salk Institute for Biological Studies, San Diego, California 92186-5800, USA.

出版信息

J Biol Chem. 1997 May 2;272(18):11757-62. doi: 10.1074/jbc.272.18.11757.

DOI:10.1074/jbc.272.18.11757
PMID:9115230
Abstract

The invariant chain (Ii) targets major histocompatibility complex class II molecules to an endocytic processing compartment where they encounter antigenic peptides. Analysis of Ii-transferrin receptor chimeras expressed in polarized Madin-Darby canine kidney (MDCK) cells shows that the Ii cytoplasmic tail contains a dihydrophobic basolateral sorting signal, Met16-Leu17, which is recognized in both the biosynthetic and endocytic pathways. Pro15-Met16-Leu17 has previously been identified as one of two dihydrophobic Ii internalization signals active in non-polarized cells. Pro15 is also required for endocytosis in MDCK cells but not for basolateral sorting, indicating that the internalization signal recognized at the plasma membrane is distinct from the sorting signal recognized by basolateral sorting machinery. Another dihydrophobic sequence, Leu7-Ile8, is required for rapid internalization of the chimeric receptors in MDCK cells but not for basolateral sorting, providing further evidence that the structural requirements for basolateral sorting and internalization differ. Deletion analysis suggests that basolateral sorting of newly synthesized Ii-TR chimeras is also mediated by the membrane-proximal region of the Ii cytoplasmic tail. However, this region does not promote polarized basolateral recycling, indicating that the structural requirements for polarized sorting in the biosynthetic and endocytic pathways are not identical.

摘要

恒定链(Ii)将主要组织相容性复合体II类分子靶向至一个内吞加工区室,在那里它们会遇到抗原肽。对在极化的犬肾Madin-Darby(MDCK)细胞中表达的Ii-转铁蛋白受体嵌合体的分析表明,Ii细胞质尾部含有一个双疏水的基底外侧分选信号,即Met16-Leu17,该信号在生物合成途径和内吞途径中均能被识别。Pro15-Met16-Leu17先前已被鉴定为在非极化细胞中起作用的两个双疏水Ii内化信号之一。Pro15对于MDCK细胞的内吞作用也是必需的,但对于基底外侧分选则不是必需的,这表明在质膜上识别的内化信号与基底外侧分选机制识别的分选信号不同。另一个双疏水序列Leu7-Ile8是MDCK细胞中嵌合受体快速内化所必需的,但对于基底外侧分选则不是必需的,这进一步证明了基底外侧分选和内化的结构要求不同。缺失分析表明,新合成的Ii-TR嵌合体的基底外侧分选也是由Ii细胞质尾部的膜近端区域介导的。然而,该区域并不能促进极化的基底外侧循环,这表明生物合成途径和内吞途径中极化分选的结构要求并不相同。

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