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牛嗜铬细胞中神经肽Y-Y1受体亚型的鉴定。

Identification of an NPY-Y1 receptor subtype in bovine chromaffin cells.

作者信息

Zhang P, Zheng J, Vorce R L, Hexum T D

机构信息

Department of Pharmacology, University of Nebraska Medical Center, Omaha 68198-6260, USA.

出版信息

Regul Pept. 2000 Feb 8;87(1-3):9-13. doi: 10.1016/s0167-0115(99)00093-2.

Abstract

Bovine chromaffin cells have been used in a variety of studies designed to reveal different aspects of neuropeptide Y (NPY) action. Pharmacological data have defined five NPY receptor subtypes, only one of which (Y3) has not been cloned. Some studies with bovine chromaffin cells have concluded that the effects of NPY on this cell type are mediated by the Y3 subtype. Previous work from our laboratory demonstrates that a Y1 subtype mediates the effect of NPY in this tissue. In the current studies we provide further evidence for the existence of the Y1 subtype in bovine chromaffin cells. BIBP3226, the selective Y1 antagonist, potently displaces [125I]NPY from its binding site IC50 = 1.91 x 10(-9) M. Moreover, [125I]BIBP3226 binds to bovine chromaffin cell membranes with high affinity (IC50 = 5.9 x 10(-8) M). Examination of BIBP3226 antagonism of NPY inhibition of forskolin stimulated cyclic AMP accumulation reveals that it is a competitive antagonist with a K(B) similar to the IC50 for [125I]BIBP3226 binding. Northern blot analysis using a porcine cDNA clone for the Y1 subtype demonstrates a 3.5-kb mRNA species in chromaffin cells. These data identify the bovine chromaffin cell NPY receptor as a Y1 subtype.

摘要

牛嗜铬细胞已被用于各种旨在揭示神经肽Y(NPY)作用不同方面的研究中。药理学数据已确定了五种NPY受体亚型,其中只有一种(Y3)尚未被克隆。一些对牛嗜铬细胞的研究得出结论,NPY对这种细胞类型的作用是由Y3亚型介导的。我们实验室之前的工作表明,Y1亚型介导了NPY在该组织中的作用。在当前的研究中,我们为牛嗜铬细胞中Y1亚型的存在提供了进一步的证据。选择性Y1拮抗剂BIBP3226能有效地将[125I]NPY从其结合位点上置换下来,IC50 = 1.91 x 10(-9) M。此外,[125I]BIBP3226以高亲和力(IC50 = 5.9 x 10(-8) M)与牛嗜铬细胞膜结合。对BIBP3226拮抗NPY抑制福斯高林刺激的环磷酸腺苷积累的研究表明,它是一种竞争性拮抗剂,其K(B)与[125I]BIBP3226结合的IC50相似。使用猪Y1亚型cDNA克隆进行的Northern印迹分析显示,嗜铬细胞中有一个3.5-kb的mRNA物种。这些数据确定牛嗜铬细胞NPY受体为Y1亚型。

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