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Interactions of GIPC with Dopamine D2 D3 but not D4 Receptors Define a Novel Mode of Regulation of G Protein-coupled Receptors

机译:GIPC与多巴胺D2D3而非D4受体的相互作用定义了G蛋白偶联受体的新型调节方式

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摘要

The C-terminus domain of G protein-coupled receptors confers a functional cytoplasmic interface involved in protein association. By screening a rat brain cDNA library using the yeast two-hybrid system with the C-terminus domain of the dopamine D3 receptor (D3R) as bait, we characterized a new interaction with the PDZ domain-containing protein, GIPC (GAIP interacting protein, C terminus). This interaction was specific for the dopamine D2 receptor (D2R) and D3R, but not for the dopamine D4 receptor (D4R) subtype. Pull-down and affinity chromatography assays confirmed this interaction with recombinant and endogenous proteins. Both GIPC mRNA and protein are widely expressed in rat brain and together with the D3R in neurons of the islands of Calleja at plasma membranes and in vesicles. GIPC reduced D3R signaling, cointernalized with D2R and D3R, and sequestered receptors in sorting vesicles to prevent their lysosomal degradation. Through its dimerization, GIPC acts as a selective scaffold protein to assist receptor functions. Our results suggest a novel function for GIPC in the maintenance, trafficking, and signaling of GPCRs.
机译:G蛋白偶联受体的C末端结构域赋予参与蛋白质缔合的功能性细胞质界面。通过使用酵母双杂交系统以多巴胺D3受体(D3R)的C末端结构域为诱饵筛选大鼠大脑cDNA文库,我们表征了与含PDZ结构域的蛋白GIPC(GAIP相互作用蛋白, C总站)。这种相互作用是特定于多巴胺D2受体(D2R)和D3R的,而不是特定于多巴胺D4受体(D4R)的亚型的。下拉和亲和色谱分析证实了这种与重组和内源蛋白的相互作用。 GIPC mRNA和蛋白质均在大鼠脑中广泛表达,并与D3R一起在质膜和囊泡的Calleja岛神经元中表达。 GIPC减少了D3R信号传导,与D2R和D3R共同内在化,并在分选小泡中隔离了受体以防止其溶酶体降解。通过其二聚化,GIPC充当选择性支架蛋白来协助受体功能。我们的结果表明,GIPC在GPCR的维持,运输和信号传导中具有新功能。

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