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首页> 外文期刊>Molecular biology of the cell >Basolateral sorting of chloride channel 2 is mediated by interactions between a dileucine motif and the clathrin adaptor AP-1
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Basolateral sorting of chloride channel 2 is mediated by interactions between a dileucine motif and the clathrin adaptor AP-1

机译:氯通道2的基底外侧分选由双亮氨酸基序与网格蛋白衔接子AP-1之间的相互作用介导

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摘要

In spite of the many key cellular functions of chloride channels, the mechanisms that mediate their subcellular localization are largely unknown. ClC-2 is a ubiquitous chloride channel usually localized to the basolateral domain of epithelia that regulates cell volume, ion transport, and acid–base balance; mice knocked out for ClC-2 are blind and sterile. Previous work suggested that CLC-2 is sorted basolaterally by TIFS812LL, a dileucine motif in CLC-2's C-terminal domain. However, our in silico modeling of ClC-2 suggested that this motif was buried within the channel's dimerization interface and identified two cytoplasmically exposed dileucine motifs, ESMI623LL and QVVA635LL, as candidate sorting signals. Alanine mutagenesis and trafficking assays support a scenario in which ESMI623LL acts as the authentic basolateral signal of ClC-2. Silencing experiments and yeast three-hybrid assays demonstrated that both ubiquitous (AP-1A) and epithelium-specific (AP-1B) forms of the tetrameric clathrin adaptor AP-1 are capable of carrying out basolateral sorting of ClC-2 through interactions of ESMI623LL with a highly conserved pocket in their γ1-σ1A hemicomplex.
机译:尽管氯化物通道具有许多关键的细胞功能,但介导其亚细胞定位的机制仍然未知。 ClC-2是一个普遍存在的氯化物通道,通常位于上皮的基底外侧区域,可调节细胞体积,离子转运和酸碱平衡。敲除ClC-2的小鼠是盲人和无菌的。先前的研究表明,CLC-2是通过TIFS 812 LL(在CLC-2的C端结构域中的双亮氨酸基序)在基底外侧进行排序的。然而,我们对ClC-2的计算机模拟表明该基序被掩埋在通道的二聚化界面中,并鉴定出两个细胞质暴露的双亮氨酸基序,即ESMI 623 LL和QVVA 635 LL ,作为候选排序信号。丙氨酸诱变和运输分析支持ESMI 623 LL作为ClC-2的真实基底外侧信号的情况。沉默实验和酵母三杂交试验表明,四聚体网格蛋白衔接子AP-1的无处不在(AP-1A)和上皮特异性(AP-1B)形式均能够通过ESMI相互作用进行ClC-2的基底外侧分选 623 LL在其γ1-σ1A半配合物中具有高度保守的口袋。

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