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位于20号染色体上的人促生长激素抑制素-14选择性受体变体(促生长激素抑制素受体4)的克隆与表达。

Cloning and expression of a human somatostatin-14-selective receptor variant (somatostatin receptor 4) located on chromosome 20.

作者信息

Demchyshyn L L, Srikant C B, Sunahara R K, Kent G, Seeman P, Van Tol H H, Panetta R, Patel Y C, Niznik H B

机构信息

Department of Psychiatry, University of Toronto, Canada.

出版信息

Mol Pharmacol. 1993 Jun;43(6):894-901.

PMID:8100352
Abstract

Based on pharmacological, biochemical, and molecular criteria, multiple somatostatin receptor (SSTR) subtypes selective for somatostatin (SST)-14 and -28 have been postulated to exist in both the brain and periphery. We report here on the cloning and characterization of a human gene encoding a new member of the guanine nucleotide-binding protein-linked SSTR family, termed human (h)SSTR4. The 388-amino acid protein, with a predicted molecular mass of approximately 42 kDa, displays sequence similarity, particularly within putative transmembrane domains, with the recently cloned hSSTR1 (69%), hSSTR2 (56%), and hSSTR3 (58%). Membranes prepared from COS-7 cells transiently expressing the hSSTR4 gene bound 125I-[Leu8,D-Trp22,Tyr25]SST-28 in a saturable manner with high affinity (approximately 60 pM) and with a pharmacological profile and rank order of potency ([D-Trp8]SST-14 > SST-14 > SMS 201-995 > SST-28 > MK-678) indicative of a SST-14-selective receptor. Ki values for the inhibition of 125I-[Leu8,D-Trp22,Tyr25]SST-28 binding to the expressed receptor by these somatostatinergic peptides were 0.3, 1.1, 1.4, 2.2, and 6.5 nM, respectively. High affinity agonist binding to hSSTR4 was significantly reduced by GTP and pertussis toxin, indicating association of the expressed receptor with pertussis toxin-sensitive guanine nucleotide-binding proteins. Northern blot analysis revealed the presence of an SSTR4 mRNA species of approximately 4 kilobases in select regions of the monkey brain, including the hippocampus, hypothalamus, cortex, and striatum, with little or no receptor mRNA detected in either the olfactory tubercle, medulla, cerebellum, or amygdala. The SSTR4 gene maps to human chromosome 20. These findings document the existence of a novel human SSTR gene. Although the hSSTR4 displays an overall deduced amino acid homology of 86% with the recently reported rat homolog [Proc. Natl. Acad. Sci. USA 89:11151-11155 (1992)], the two gene products possess distinctive pharmacological profiles and affinities for the SST agonists SMS 201-995 and MK-678.

摘要

基于药理学、生物化学及分子标准,已推测在脑和外周均存在对生长抑素(SST)-14和-28具有选择性的多种生长抑素受体(SSTR)亚型。我们在此报告一个编码鸟嘌呤核苷酸结合蛋白偶联SSTR家族新成员的人类基因的克隆及特性分析,该新成员被命名为人类(h)SSTR4。这个由388个氨基酸组成的蛋白质,预测分子量约为42 kDa,与最近克隆的hSSTR1(69%)、hSSTR2(56%)和hSSTR3(58%)显示出序列相似性,尤其是在假定的跨膜结构域内。从瞬时表达hSSTR4基因的COS-7细胞制备的膜以高亲和力(约60 pM)以可饱和方式结合125I-[亮氨酸8,D-色氨酸22,酪氨酸25]SST-28,其药理学特征和效价顺序([D-色氨酸8]SST-14 > SST-14 > SMS 201-995 > SST-28 > MK-678)表明是一种SST-14选择性受体。这些生长抑素能肽抑制125I-[亮氨酸8,D-色氨酸22,酪氨酸25]SST-28与表达受体结合的Ki值分别为0.3、1.1、1.4、2.2和6.5 nM。GTP和百日咳毒素显著降低了高亲和力激动剂与hSSTR4的结合,表明表达的受体与百日咳毒素敏感的鸟嘌呤核苷酸结合蛋白相关。Northern印迹分析显示在猴脑的特定区域,包括海马体、下丘脑、皮层和纹状体,存在一种约4千碱基的SSTR4 mRNA,而在嗅结节、延髓、小脑或杏仁核中几乎未检测到受体mRNA。SSTR4基因定位于人类20号染色体。这些发现证明了一种新型人类SSTR基因的存在。尽管hSSTR4与最近报道的大鼠同源物[美国国家科学院院刊89:11151-11155(1992)]显示出86%的总体推导氨基酸同源性,但这两种基因产物对SST激动剂SMS 201-995和MK-678具有独特的药理学特征和亲和力。

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