Parker S L, Parker M S, Sah R, Sallee F R, Balasubramaniam A
Department of Pharmacology, University of Tennessee Health Science Center, Memphis, TN 38163, USA.
Regul Pept. 2007 Mar 1;139(1-3):128-35. doi: 10.1016/j.regpep.2006.10.014. Epub 2006 Dec 18.
The Y(2) receptor for neuropeptide Y (NPY) interacts with pertussis toxin (PTX)-sensitive G-proteins, but little is known about interdependence of their levels and functions. We found that PTX reduces Y(2) receptors expressed in CHO cells in parallel to inactivation of Gi G-proteins, to loss of inhibition by Y(2) agonists of forskolin-stimulated adenylyl cyclase, and to decrease in the binding of GTP-gamma-S. These losses were attenuated by the endosome alkalinizer ammonium chloride. Affinity of the Y(2) receptor was not changed by PTX treatment. Prolonged treatment induced a large decrease of Y(2) receptor immunoreactivity (more than 70% in 48 h). The Gi(3) alpha-subunit immunoreactivity decreased slowly (about 46% in 48 h). There was a significant increase in Gq alpha immunoreactivity and in fraction of Y(2) binding sensitive to a Gq-selective antagonist. Possibly linked to that, the surface Y(2) sites and the internalization of the Y(2) receptor were less than 40% reduced. However, the abundant masked Y(2) sites were eliminated by the toxin, and could be mainly coupled to PTX-sensitive G-proteins.
神经肽Y(NPY)的Y(2)受体与百日咳毒素(PTX)敏感的G蛋白相互作用,但其水平和功能的相互依赖性却鲜为人知。我们发现,PTX可使CHO细胞中表达的Y(2)受体减少,同时Gi G蛋白失活,Y(2)激动剂对福斯高林刺激的腺苷酸环化酶的抑制作用丧失,以及GTP-γ-S结合减少。这些损失可被内体碱化剂氯化铵减弱。PTX处理不会改变Y(2)受体的亲和力。长时间处理会导致Y(2)受体免疫反应性大幅下降(48小时内超过70%)。Gi(3)α亚基免疫反应性缓慢下降(48小时内约46%)。Gqα免疫反应性以及对Gq选择性拮抗剂敏感的Y(2)结合部分显著增加。这可能与之相关,表面Y(2)位点和Y(2)受体的内化减少不到40%。然而,大量被掩盖的Y(2)位点被毒素消除,且可能主要与PTX敏感的G蛋白偶联。
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