Massotte Dominique, Brillet Karl, Kieffer Brigitte, Milligan Graeme
Département des Récepteurs et Protéines Membranaires, CNRS UPR 9050, Ecole Supérieure de Biotechnologie de Strasbourg, Illkirch-Graffenstaden, France.
J Neurochem. 2002 Jun;81(6):1372-82. doi: 10.1046/j.1471-4159.2002.00946.x.
As preferential coupling of opioid receptor to various inhibitory Galpha subunits is still under debate, we have investigated the selectivity of the human mu opioid receptor fused to a pertussis toxin insensitive C351I Gi1 alpha or C352I Gi2 alpha in stably transfected HEK 293 cells. Overall agonist binding affinities were increased for both fusion constructs when compared to the wild type receptor. [35 S]GTPgammaS binding was performed on pertussis toxin treated cells to monitor coupling efficiency of the fusion constructs. Upon agonist addition hMOR-C351I Gi1 a exhibited an activation profile similar to the non-fused receptor while hMOR-C352I Gi2 alpha was poorly activated. Interestingly no correlation could be drawn between agonist binding affinity and efficacy. Upon agonist addition, forskolin-stimulated cAMP production, as measured using a reporter gene assay, was inhibited by signals transduced via the fused Gi1 alpha and Gi2 alpha mainly. In contrast both fusion constructs were able to initiate ERK-MAPK phosphorylation via coupling to endogenous G proteins only. In conclusion our data indicate that hMOR couples more efficiently to Gi1 alpha than Gi2 alpha and that the coupling efficacy is clearly agonist-dependent.
由于阿片受体与各种抑制性Gα亚基的优先偶联仍存在争议,我们研究了在稳定转染的HEK 293细胞中,与百日咳毒素不敏感的C351I Gi1α或C352I Gi2α融合的人μ阿片受体的选择性。与野生型受体相比,两种融合构建体的总体激动剂结合亲和力均有所增加。在百日咳毒素处理的细胞上进行[35S]GTPγS结合,以监测融合构建体的偶联效率。加入激动剂后,hMOR-C351I Gi1α表现出与未融合受体相似的激活曲线,而hMOR-C352I Gi2α的激活较差。有趣的是,激动剂结合亲和力与效力之间没有相关性。加入激动剂后,使用报告基因测定法测量的福斯高林刺激的cAMP产生主要受到通过融合的Gi1α和Gi2α转导的信号的抑制。相比之下,两种融合构建体仅通过与内源性G蛋白偶联就能启动ERK-MAPK磷酸化。总之,我们的数据表明,hMOR与Gi1α的偶联比与Gi2α更有效,并且偶联效率明显依赖于激动剂。
