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在马-达二氏犬肾细胞中,主要组织相容性复合体II类分子的极化运输由β链胞质尾部基于亮氨酸的信号引导。

Polarized transport of MHC class II molecules in Madin-Darby canine kidney cells is directed by a leucine-based signal in the cytoplasmic tail of the beta-chain.

作者信息

Simonsen A, Pedersen K W, Nordeng T W, von der Lippe A, Stang E, Long E O, Bakke O

机构信息

Department of Biology, University of Oslo, Norway.

出版信息

J Immunol. 1999 Sep 1;163(5):2540-8.

Abstract

MHC class II molecules are found on the basolateral plasma membrane domain of polarized epithelial cells, where they can present Ag to intraepithelial lymphocytes in the vascular space. We have analyzed the sorting information required for efficient intracellular localization and polarized distribution of MHC class II molecules in stably transfected Madin-Darby canine kidney cells. These cells were able to present influenza virus particles to HLA-DR1-restricted T cell clones. Wild-type MHC class II molecules were located on the basolateral plasma membrane domain, in basolateral early endosomes, and in late multivesicular endosomes, the latter also containing the MHC class II-associated invariant chain and an HLA-DM fusion protein. A phenylalanine-leucine residue within the cytoplasmic tail of the beta-chain was required for basolateral distribution, efficient internalization, and localization of the MHC class II molecules to basolateral early endosomes. However, distribution to apically located, late multivesicular endosomes did not depend on signals in the class II cytoplasmic tails as both wild-type class II molecules and mutant molecules lacking the phenylalanine-leucine motif were found in these compartments. Our results demonstrate that sorting information in the tails of class II dimers is an absolute requirement for their basolateral surface distribution and intracellular localization.

摘要

MHC II类分子存在于极化上皮细胞的基底外侧质膜结构域,在那里它们可以将抗原呈递给血管腔内的上皮内淋巴细胞。我们分析了稳定转染的Madin-Darby犬肾细胞中MHC II类分子有效细胞内定位和极化分布所需的分选信息。这些细胞能够将流感病毒颗粒呈递给HLA-DR1限制性T细胞克隆。野生型MHC II类分子位于基底外侧质膜结构域、基底外侧早期内体和晚期多泡内体中,后者还含有与MHC II类相关的恒定链和一种HLA-DM融合蛋白。β链胞质尾内的苯丙氨酸-亮氨酸残基是MHC II类分子基底外侧分布、有效内化以及定位于基底外侧早期内体所必需的。然而,定位于顶端的晚期多泡内体的分布并不依赖于II类胞质尾中的信号,因为在这些区室中发现了野生型II类分子和缺乏苯丙氨酸-亮氨酸基序的突变分子。我们的结果表明,II类二聚体尾中的分选信息是其基底外侧表面分布和细胞内定位的绝对必要条件。

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