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The Serotonin Transporter Is an Exclusive Client of the Coat Protein Complex II (COPII) Component SEC24C*

机译:血清素转运蛋白是外壳蛋白复合物II(COPII)组分SEC24C的独家客户*

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摘要

The transporters for serotonin (SERT), dopamine, and noradrenaline have a conserved hydrophobic core but divergent N and C termini. The C terminus harbors the binding site for the coat protein complex II (COPII) cargo-binding protein SEC24. Here we explored which SEC24 isoform was required for export of SERT from the endoplasmic reticulum (ER). Three lines of evidence argue that SERT can only exit the ER by recruiting SEC24C: (i) Mass spectrometry showed that a peptide corresponding to the C terminus of SERT recruited SEC24C-containing COPII complexes from mouse brain lysates. (ii) Depletion of individual SEC24 isoforms by siRNAs revealed that SERT was trapped in the ER only if SEC24C was down-regulated, in both, cells that expressed SERT endogenously or after transfection. The combination of all siRNAs was not more effective than that directed against SEC24C. A SERT mutant in which the SEC24C-binding motif (607RI608) was replaced by alanine was insensitive to down-regulation of SEC24C levels. (iii) Overexpression of a SEC24C variant with a mutation in the candidate cargo-binding motif (SEC24C-D796V/D797N) but not of the corresponding mutant SEC24D-D733V/D734N reduced SERT surface levels. In contrast, noradrenaline and dopamine transporters and the more distantly related GABA transporter 1 relied on SEC24D for ER export. These observations demonstrate that closely related transporters are exclusive client cargo proteins for different SEC24 isoforms. The short promoter polymorphism results in reduced SERT cell surface levels and renders affected individuals more susceptible to depression. By inference, variations in the Sec24C gene may also affect SERT cell surface levels and thus be linked to mood disorders.
机译:血清素(SERT),多巴胺和去甲肾上腺素的转运蛋白具有保守的疏水核心,但N和C末端有差异。 C末端带有外壳蛋白复合物II(COPII)货物结合蛋白SEC24的结合位点。在这里,我们探讨了从内质网(ER)出口SERT所需的SEC24亚型。三个证据表明,SERT只能通过募集SEC24C才能退出ER:(i)质谱显示,与SERT C末端相对应的肽从小鼠脑裂解物中募集了包含SEC24C的COPII复合物。 (ii)siRNA消耗单个SEC24同工型表明,只有在内源表达SERT或转染后均表达SERT的两种细胞中,只有SEC24C下调时,SERT才会被捕获在ER中。所有siRNA的结合并不比针对SEC24C的结合更有效。其中SEC24C结合基序(607RI608)被丙氨酸取代的SERT突变体对SEC24C水平的下调不敏感。 (iii)在候选货物结合基序中有突变的SEC24C变体(SEC24C-D796V / D797N)的过表达,但没有相应的突变SEC24D-D733V / D734N的突变,则降低了SERT表面水平。相比之下,去甲肾上腺素和多巴胺转运蛋白以及更远相关的GABA转运蛋白1依靠SEC24D进行ER出口。这些观察表明,密切相关的转运蛋白是不同SEC24同工型的排他性客货运蛋白。短启动子多态性导致SERT细胞表面水平降低,并使受影响的个体更容易抑郁。通过推断,Sec24C基因的变异也可能影响SERT细胞表面水平,因此与情绪障碍有关。

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