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异源表达的哺乳动物嗅觉受体的配体选择性激活

Ligand-selective activation of heterologously-expressed mammalian olfactory receptor.

作者信息

Ukhanov K, Bobkov Y, Corey E A, Ache B W

机构信息

Whitney Laboratory, Center for Smell and Taste, and McKnight Brain Institute, University of Florida, Gainesville, FL 32610, United States.

Whitney Laboratory, Center for Smell and Taste, and McKnight Brain Institute, University of Florida, Gainesville, FL 32610, United States.

出版信息

Cell Calcium. 2014 Oct;56(4):245-56. doi: 10.1016/j.ceca.2014.07.012. Epub 2014 Aug 4.

Abstract

Mammalian olfactory receptors (ORs) appear to have the capacity to couple to multiple G protein-coupled signaling pathways in a ligand-dependent selective manner. To better understand the mechanisms and molecular range of such ligand selectivity, we expressed the mouse eugenol OR (mOR-EG) in HEK293T cells together with Gα15 to monitor activation of the phospholipase-C (PLC) signaling pathway and/or Gαolf to monitor activation of the adenylate cyclase (AC) signaling pathway, resulting in intracellular Ca(2+) release and/or Ca(2+) influx through a cyclic nucleotide-gated channel, respectively. PLC-dependent responses differed dynamically from AC-dependent responses, allowing them to be distinguished when Gα15 and Gαolf were co-expressed. The dynamic difference in readout was independent of the receptor, the heterologous expression system, and the ligand concentration. Of 17 reported mOR-EG ligands tested, including eugenol, its analogs, and structurally dissimilar compounds (mousse cristal, nootkatone, orivone), some equally activated both signaling pathways, some differentially activated both signaling pathways, and some had no noticeable effect even at 1-5mM. Our findings argue that mOR-EG, when heterologously expressed, can couple to two different signaling pathways in a ligand selective manner. The challenge now is to determine the potential of mOR-EG, and perhaps other ORs, to activate multiple signaling pathways in a ligand selective manner in native ORNs.

摘要

哺乳动物嗅觉受体(ORs)似乎有能力以配体依赖的选择性方式与多种G蛋白偶联信号通路相结合。为了更好地理解这种配体选择性的机制和分子范围,我们在HEK293T细胞中共同表达小鼠丁香酚OR(mOR-EG)和Gα15,以监测磷脂酶C(PLC)信号通路的激活,和/或共同表达Gαolf以监测腺苷酸环化酶(AC)信号通路的激活,分别导致细胞内Ca(2+)释放和/或通过环核苷酸门控通道的Ca(2+)内流。PLC依赖性反应与AC依赖性反应在动力学上有所不同,当共同表达Gα15和Gαolf时可以区分它们。读出信号的动力学差异与受体、异源表达系统和配体浓度无关。在测试的17种已报道的mOR-EG配体中,包括丁香酚及其类似物,以及结构不同的化合物(慕斯水晶、诺卡酮、奥里冯),一些配体同等程度地激活了两条信号通路,一些配体差异性地激活了两条信号通路,还有一些即使在1-5mM浓度下也没有明显作用。我们的研究结果表明,mOR-EG在异源表达时能够以配体选择性的方式与两种不同的信号通路相结合。现在的挑战是确定mOR-EG以及或许其他ORs在天然嗅觉感受神经元中以配体选择性方式激活多种信号通路的潜力。

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