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蛙皮素在小鼠结肠黏膜膜上的高亲和力结合位点。

High-affinity binding sites for bombesin on mouse colonic mucosal membranes.

作者信息

Narayan S, Draviam E, Rajaraman S, Singh P

机构信息

Department of Surgery, University of Texas Medical Branch, Galveston 77550.

出版信息

Mol Cell Biochem. 1991 Jul 24;106(1):31-9. doi: 10.1007/BF00231186.

DOI:10.1007/BF00231186
PMID:1656207
Abstract

Bombesin (BBS) has specific biological effects on colonic mucosal cells, but the presence of BBS receptors on colonic mucosa have not been described to-date. In the present study we examined the mouse colonic mucosal membranes for the presence of specific binding sites for BBS/gastrin releasing peptides (GRP), and characterized the binding kinetics and molecular weight of the specific binding proteins. The radiolabeled ligand (125I-Tyr4-BBS), in the absence or presence of a 1000-fold excess of BBS, was used to establish the optimal binding assay conditions of time, pH and temperature for measuring the maximum number of specific binding sites for BBS related peptides. Under the optimal binding assay conditions, BBS displaced the binding of 125I-Tyr4-BBS in a dose-related manner. A single class of high-affinity binding sites (Kd = 0.23 +/- 0.02 nM) for BBS were measured, with a binding capacity of 27.3 +/- 4.6 fmoles/mg membrane protein. The binding sites were specific for binding BBS/GRP related peptides, since all structurally related peptides inhibited the binding of 125I-Tyr4-BBS in a dose-dependent manner, while structurally unrelated peptides did not compete for the 125I-Tyr4-BBS binding sites. The relative binding affinity (RBA) of BBS/GRP related peptides was determined to be in the order of GRP (14-27) = GRP (18-27) greater than GRP (1-27) greater than neuromedin B greater than BBS. The BBS-receptor antagonists, [Leu13-psi-(CH2NH) Leu14]-BBS (LL-BBS) and D-Phe6, BN(6-13) propylamide (D-Phe6, BN(6-13)-PA), inhibited the specific binding of 125I-Tyr4-BBS to colonic mucosal membranes in a dose-dependent manner.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

蛙皮素(BBS)对结肠黏膜细胞具有特定的生物学效应,但迄今为止,尚未有关于结肠黏膜上存在BBS受体的描述。在本研究中,我们检测了小鼠结肠黏膜膜上是否存在BBS/胃泌素释放肽(GRP)的特异性结合位点,并对特异性结合蛋白的结合动力学和分子量进行了表征。使用放射性标记配体(125I-Tyr4-BBS),在不存在或存在1000倍过量BBS的情况下,确定用于测量BBS相关肽特异性结合位点最大数量的时间、pH和温度的最佳结合测定条件。在最佳结合测定条件下,BBS以剂量相关的方式取代125I-Tyr4-BBS的结合。测量到一类针对BBS的高亲和力结合位点(Kd = 0.23 +/- 0.02 nM),结合容量为27.3 +/- 4.6 fmol/mg膜蛋白。这些结合位点对结合BBS/GRP相关肽具有特异性,因为所有结构相关肽均以剂量依赖性方式抑制125I-Tyr4-BBS的结合,而结构不相关肽不竞争125I-Tyr4-BBS结合位点。BBS/GRP相关肽的相对结合亲和力(RBA)确定为GRP(14-27)= GRP(18-27)大于GRP(1-27)大于神经降压素B大于BBS。BBS受体拮抗剂[Leu13-psi-(CH2NH)Leu14]-BBS(LL-BBS)和D-Phe6,BN(6-13)丙酰胺(D-Phe6,BN(6-13)-PA)以剂量依赖性方式抑制125I-Tyr4-BBS与结肠黏膜膜的特异性结合。(摘要截断于250字)

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2
Characterization of gastrin binding to colonic mucosal membranes of guinea pigs.
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本文引用的文献

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Protein measurement with the Folin phenol reagent.使用福林酚试剂进行蛋白质测定。
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