首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Olfactory receptor surface expression is driven by association with the beta(2)-adrenergic receptor
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Olfactory receptor surface expression is driven by association with the beta(2)-adrenergic receptor

机译:嗅觉受体表面表达是由与β(2)-肾上腺素受体的结合驱动的

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Olfactory receptors (ORs) comprise more than half of the large class I G protein-coupled receptor (GPCR) superfamily. Although cloned over a decade ago, little is known about their properties because wild-type ORs do not efficiently reach the cell surface following heterologous expression. Receptor-receptor interactions strongly influence surface trafficking of other GPCRs, and we examined whether a similar mechanism might be involved in OR surface expression. Olfactory neurons are known to express beta-adrenergic receptors (ARs), and we found that coexpression with beta(2)-ARs, but not any other AR subtypes, dramatically increased mouse 71 (M71) OR surface expression in human embryonic kidney 293 cells. A persistent physical interaction between M71 ORs and beta(2)-ARs was shown by coimmunoprecipitation and by cointernalization of the two receptors in response to their specific ligands. Also, coexpression of wild-type M71 ORs with beta(2)-ARs resulted in cAMP responses to the M71 ligand acetophenone. Finally, in situ hybridization studies showed extensive colocalization of M71 OR and beta(2)-AR expression in mouse olfactory epithelium. These data demonstrate the successful heterologous surface expression of a functional wild-type OR and reveal that persistent physical association with other GPCRs can control OR surface expression.
机译:嗅觉受体(OR)占大型I G蛋白偶联受体(GPCR)超家族的一半以上。尽管已经克隆了十多年,但对其性质了解甚少,因为野生型OR在异​​源表达后不能有效地到达细胞表面。受体之间的相互作用强烈影响其他GPCR的表面运输,我们研究了OR表面表达是否可能涉及类似的机制。嗅觉神经元已知表达β-肾上腺素能受体(ARs),我们发现与beta(2)-ARs共表达,但未与其他AR亚型共表达,可大大增加人类胚胎肾脏293细胞中的小鼠71(M71)或表面表达。 M71 OR和beta(2)-ARs之间的持久性物理相互作用通过共免疫沉淀法和通过响应这两种受体的特定配体的共内化作用来显示。同样,野生型M71 OR与beta(2)-ARs的共表达导致cAMP对M71配体苯乙酮的响应。最后,原位杂交研究显示在小鼠嗅觉上皮细胞中M71 OR和beta(2)-AR表达广泛共定位。这些数据证明了功能性野生型OR的成功异源表面表达,并揭示了与其他GPCR的持久性物理缔合可以控制OR表面表达。

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