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本文引用的文献

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Transcytosis of NgCAM in epithelial cells reflects differential signal recognition on the endocytic and secretory pathways.NgCAM在上皮细胞中的转胞吞作用反映了内吞和分泌途径上不同的信号识别。
J Cell Biol. 2005 Aug 15;170(4):595-605. doi: 10.1083/jcb.200506051. Epub 2005 Aug 8.
2
Non-canonical YXXGPhi endocytic motifs: recognition by AP2 and preferential utilization in P2X4 receptors.非典型YXXGPhi内吞基序:被AP2识别并在P2X4受体中优先利用。
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Recycling endosomes can serve as intermediates during transport from the Golgi to the plasma membrane of MDCK cells.回收型内体可在从高尔基体到MDCK细胞质膜的运输过程中充当中间体。
J Cell Biol. 2004 Nov 8;167(3):531-43. doi: 10.1083/jcb.200408165.
4
The basolateral targeting signal of CD147 (EMMPRIN) consists of a single leucine and is not recognized by retinal pigment epithelium.CD147(细胞外基质金属蛋白酶诱导因子)的基底外侧靶向信号由单个亮氨酸组成,且不被视网膜色素上皮识别。
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Sorting of H,K-ATPase beta-subunit in MDCK and LLC-PK cells is independent of mu 1B adaptin expression.H,K - ATP酶β亚基在MDCK和LLC - PK细胞中的分选与μ1B衔接蛋白的表达无关。
Traffic. 2004 Jun;5(6):449-61. doi: 10.1111/j.1398-9219.2004.00192.x.
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The COOH-terminal tail of the GAT-2 GABA transporter contains a novel motif that plays a role in basolateral targeting.GAT-2γ-氨基丁酸转运体的羧基末端尾巴包含一个在基底外侧靶向中起作用的新基序。
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Delivery of raft-associated, GPI-anchored proteins to the apical surface of polarized MDCK cells by a transcytotic pathway.通过转胞吞途径将筏相关的糖基磷脂酰肌醇锚定蛋白递送至极化的MDCK细胞的顶端表面。
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Targeting of membrane proteins to endosomes and lysosomes.将膜蛋白靶向内体和溶酶体。
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The GGA proteins: adaptors on the move.GGA蛋白:移动中的衔接蛋白。
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AP-1B: polarized sorting at the endosome.AP-1B:在内体进行极化分选。
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跨膜蛋白shrew-1靶向黏着连接是由细胞质分选基序控制的。

Targeting of transmembrane protein shrew-1 to adherens junctions is controlled by cytoplasmic sorting motifs.

作者信息

Jakob Viktor, Schreiner Alexander, Tikkanen Ritva, Starzinski-Powitz Anna

机构信息

Institute of Cell Biology and Neuroscience, Johann-Wolfgang Goethe University of Frankfurt, D-60323 Frankfurt am Main, Germany.

出版信息

Mol Biol Cell. 2006 Aug;17(8):3397-408. doi: 10.1091/mbc.e05-11-1034. Epub 2006 May 17.

DOI:10.1091/mbc.e05-11-1034
PMID:16707570
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1525240/
Abstract

We recently identified transmembrane protein shrew-1 and showed that it is able to target to adherens junctions in polarized epithelial cells. This suggested shrew-1 possesses specific basolateral sorting motifs, which we analyzed by mutational analysis. Systematic mutation of amino acids in putative sorting signals in the cytoplasmic domain of shrew-1 revealed three tyrosines and a dileucine motif necessary for basolateral sorting. Substitution of these amino acids leads to apical localization of shrew-1. By applying tannic acid to either the apical or basolateral part of polarized epithelial cells, thereby blocking vesicle fusion with the plasma membrane, we obtained evidence that the apically localized mutants were primarily targeted to the basolateral membrane and were then redistributed to the apical domain. Further support for a postendocytic sorting mechanism of shrew-1 was obtained by demonstrating that mu1B, a subunit of the epithelial cell-specific adaptor complex AP-1B, interacts with shrew-1. In conclusion, our data provide evidence for a scenario where shrew-1 is primarily delivered to the basolateral membrane by a so far unknown mechanism. Once there, adaptor protein complex AP-1B is involved in retaining shrew-1 at the basolateral membrane by postendocytic sorting mechanisms.

摘要

我们最近鉴定出跨膜蛋白shrew-1,并表明它能够靶向极化上皮细胞中的黏着连接。这表明shrew-1具有特定的基底外侧分选基序,我们通过突变分析对其进行了研究。对shrew-1细胞质结构域中假定分选信号的氨基酸进行系统突变,揭示了基底外侧分选所需的三个酪氨酸和一个双亮氨酸基序。这些氨基酸的替换导致shrew-1定位于顶端。通过将单宁酸应用于极化上皮细胞的顶端或基底外侧部分,从而阻断囊泡与质膜的融合,我们获得了证据,即顶端定位的突变体主要靶向基底外侧膜,然后重新分布到顶端结构域。通过证明上皮细胞特异性衔接蛋白复合物AP-1B的一个亚基mu1B与shrew-1相互作用,进一步支持了shrew-1内吞后分选机制。总之,我们的数据为这样一种情况提供了证据,即shrew-1主要通过一种迄今未知的机制被递送到基底外侧膜。一旦到达那里,衔接蛋白复合物AP-1B通过内吞后分选机制参与将shrew-1保留在基底外侧膜上。