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亚型选择性生长抑素受体激动剂的鉴定与表征

Identification and characterization of subtype selective somatostatin receptor agonists.

作者信息

Rohrer S P, Schaeffer J M

机构信息

Department of Endocrinology and Chemical Biology, Merck Research Laboratories, Rahway, NJ 07065, USA.

出版信息

J Physiol Paris. 2000 May-Aug;94(3-4):211-5. doi: 10.1016/s0928-4257(00)00215-1.

Abstract

High affinity, subtype selective non-peptide agonists of somatostatin receptor subtypes 1-5 were identified in combinatorial libraries constructed based on molecular modeling of known peptide agonists. Simultaneous traditional chemical synthesis yielded an additional series of somatostatin subtype-2 receptor (SSTR2) selective agonists. These compounds have been used to further define the physiological functions of the individual somatostatin receptor subtypes. In vitro experiments demonstrated the role of the SSTR2 in inhibition of glucagon release from mouse pancreatic alpha-cells and the somatostatin subtype-5 receptor (SSTR5) as a mediator of insulin secretion from pancreatic beta-cells. Both SSTR2 and SSTR5 regulated growth hormone release from the rat anterior pituitary gland. In vivo studies performed with SSTR2 receptor selective compounds demonstrated effective inhibition of pulsatile growth hormone release in rats. The SSTR2 selective compounds also lowered plasma glucose levels in normal and diabetic animal models. The availability of high affinity, subtype selective non-peptide agonists for each of the somatostatin receptors provides a direct approach to defining their physiological function both peripherally and in the central nervous system.

摘要

基于已知肽类激动剂的分子模型构建组合文库,从中鉴定出了生长抑素受体亚型1 - 5的高亲和力、亚型选择性非肽类激动剂。同时,传统化学合成产生了另一系列生长抑素2型受体(SSTR2)选择性激动剂。这些化合物已被用于进一步明确各个生长抑素受体亚型的生理功能。体外实验证明,SSTR2在抑制小鼠胰腺α细胞释放胰高血糖素中发挥作用,而生长抑素5型受体(SSTR5)作为胰腺β细胞胰岛素分泌的介质。SSTR2和SSTR5均调节大鼠垂体前叶释放生长激素。使用SSTR2受体选择性化合物进行的体内研究表明,其能有效抑制大鼠脉冲式生长激素释放。SSTR2选择性化合物还降低了正常和糖尿病动物模型的血糖水平。针对每种生长抑素受体的高亲和力、亚型选择性非肽类激动剂的可得性,为在外周和中枢神经系统中明确其生理功能提供了直接途径。

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