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神经元ClC-3剪接变体在亚细胞定位上存在差异,但介导相同的转运功能。

Neuronal ClC-3 Splice Variants Differ in Subcellular Localizations, but Mediate Identical Transport Functions.

作者信息

Guzman Raul E, Miranda-Laferte Erick, Franzen Arne, Fahlke Christoph

机构信息

From the Institute of Complex Systems, Zelluläre Biophysik (ICS-4), Forschungszentrum Jülich, 52425 Jülich, Germany

From the Institute of Complex Systems, Zelluläre Biophysik (ICS-4), Forschungszentrum Jülich, 52425 Jülich, Germany.

出版信息

J Biol Chem. 2015 Oct 23;290(43):25851-62. doi: 10.1074/jbc.M115.668186. Epub 2015 Sep 4.

Abstract

ClC-3 is a member of the CLC family of anion channels and transporters, for which multiple functional properties and subcellular localizations have been reported. Since alternative splicing often results in proteins with diverse properties, we investigated to what extent alternative splicing might influence subcellular targeting and function of ClC-3. We identified three alternatively spliced ClC-3 isoforms, ClC-3a, ClC-3b, and ClC-3c, in mouse brain, with ClC-3c being the predominant splice variant. Whereas ClC-3a and ClC-3b are present in late endosomes/lysosomes, ClC-3c is targeted to recycling endosomes via a novel N-terminal isoleucine-proline (IP) motif. Surface membrane insertion of a fraction of ClC-3c transporters permitted electrophysiological characterization of this splice variant through whole-cell patch clamping on transfected mammalian cells. In contrast, neutralization of the N-terminal dileucine-like motifs was required for functional analysis of ClC-3a and ClC-3b. Heterologous expression of ClC-3a or ClC-3b carrying mutations in N-terminal dileucine motifs as well as WTClC-3c in HEK293T cells resulted in outwardly rectifying Cl(-) currents with significant capacitive current components. We conclude that alternative splicing of Clcn3 results in proteins with different subcellular localizations, but leaves the transport function of the proteins unaffected.

摘要

ClC-3是阴离子通道和转运体的CLC家族成员,已有多种关于其功能特性和亚细胞定位的报道。由于可变剪接常常产生具有不同特性的蛋白质,我们研究了可变剪接在多大程度上可能影响ClC-3的亚细胞靶向和功能。我们在小鼠大脑中鉴定出三种可变剪接的ClC-3亚型,即ClC-3a、ClC-3b和ClC-3c,其中ClC-3c是主要的剪接变体。ClC-3a和ClC-3b存在于晚期内体/溶酶体中,而ClC-3c通过一个新的N端异亮氨酸-脯氨酸(IP)基序靶向至再循环内体。一部分ClC-3c转运体插入到细胞膜表面,从而可以通过对转染的哺乳动物细胞进行全细胞膜片钳记录来对该剪接变体进行电生理特性分析。相比之下,对ClC-3a和ClC-3b进行功能分析则需要中和其N端双亮氨酸样基序。在HEK293T细胞中异源表达N端双亮氨酸基序携带突变的ClC-3a或ClC-3b以及野生型ClC-3c,会产生外向整流的Cl(-)电流,并伴有明显的电容性电流成分。我们得出结论,Clcn3的可变剪接产生了具有不同亚细胞定位的蛋白质,但并未影响这些蛋白质的转运功能。

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