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首页> 外文期刊>Regulatory peptides. >Oligomerization of neuropeptide Y (NPY) Y2 receptors in CHO cells depends on functional pertussis toxin-sensitive G-proteins.
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Oligomerization of neuropeptide Y (NPY) Y2 receptors in CHO cells depends on functional pertussis toxin-sensitive G-proteins.

机译:CHO细胞中神经肽Y(NPY)Y2受体的低聚取决于功能性百日咳毒素敏感的G蛋白。

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摘要

Human neuropeptide Y Y2 receptors expressed in CHO cells are largely oligomeric, and upon solubilization are recovered by density gradient centrifugation as approximately 180 kDa complexes of receptor dimers and G-protein heterotrimers. A large fraction of the receptors is inactivated in the presence of pertussis toxin, in parallel with inactivation of Gi alpha subunits (with half-periods of about 4 h for both). This is accompanied by a very long-lasting loss of receptor dimers and of masked surface Y2 sites (an apparent receptor reserve pre-coupled mainly to Gi alpha subunit-containing G-proteins). However, surface Y2 receptors accessible to large peptide agonists are much less sensitive to the toxin. All surface Y2 receptors are rapidly blocked by Y2 antagonist BIIE0246, with a significant loss of the dimers, but with little change of basal Gi activity. However, both dimers and Y2 receptor compartmentalization are restored within 24 h after removal of the antagonist. In CHO cells, the maintenance andorganization of Y2 receptors appear to critically depend on functional pertussis toxin-sensitive G-proteins.
机译:在CHO细胞中表达的人神经肽Y Y2受体大部分为寡聚体,溶解后通过密度梯度离心回收为约180 kDa的受体二聚体和G蛋白异源三聚体。在百日咳毒素的存在下,大部分受体被灭活,与Giα亚基的灭活平行(两者的半周期约为4小时)。这伴随着受体二聚体和被掩盖的表面Y2位点(表观的受体储备主要与含Giα亚基的G蛋白预偶联)的非常持久的损失。但是,大型肽激动剂可及的表面Y2受体对毒素的敏感性要低得多。所有表面Y2受体均被Y2拮抗剂BIIE0246快速阻断,二聚体明显损失,但基础Gi活性几乎没有变化。然而,二聚体和Y 2受体的区室化都在去除拮抗剂后24小时内恢复。在CHO细胞中,Y2受体的维持和组织似乎主要取决于功能性百日咳毒素敏感的G蛋白。

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