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神经降压素两个N端片段神经降压素1-8和神经降压素1-10的生物活性证据。

Evidence for biological activity of two N-terminal fragments of neurotensin, neurotensin1-8 and neurotensin1-10.

作者信息

Hernandez D E, Richardson C M, Nemeroff C B, Orlando R C, St-Pierre S, Rioux F, Prange A J

出版信息

Brain Res. 1984 May 28;301(1):153-6. doi: 10.1016/0006-8993(84)90414-1.

Abstract

Intracisternal (i.c.) administration of the endogenous tridecapeptide neurotensin (NT) has been previously shown to significantly reduce the incidence of cold-restraint stress (CRS)-induced gastric ulcers in rats. In this study we confirm the cytoprotective activity of central NT, and document structure-activity relationships for this effect of NT. When tested in a dose equimolar to 17.9 nmol of NT the NT analogs [Gln4]NT, D-Trp11-NT, and D-Arg8-NT were cytoprotective, whereas D-Arg9-NT was not. Gonadotropin-releasing hormone (Gn-RH) and melanocyte-stimulating hormone-release inhibiting factor (MIF-1), two oligopeptides structurally unrelated to NT exhibited no cytoprotective efficacy in this paradigm. The C-terminal fragments of NT, xenopsin and NT8-13, and the N-terminal fragment NT1-6 were completely ineffective. Finally, NT1-8 and NT1-10, two N-terminal fragments of NT produced significant cytoprotective activity at this dose level. The cytoprotection afforded by NT1-8 and NT1-10, like that of NT, was dose-dependent with ED50's similar to that of NT (NT = 16.2 nmol, NT1-8 = 17.8 nmol and NT1-10 = 19.9 nmol). In conclusion, we demonstrate that smaller molecular weight forms of NT thought to be degradation products of NT can effectively exert biological effects.

摘要

先前已表明,向大鼠脑池内(i.c.)注射内源性十三肽神经降压素(NT)可显著降低冷束缚应激(CRS)诱导的胃溃疡发生率。在本研究中,我们证实了中枢NT的细胞保护活性,并记录了NT这种作用的构效关系。当以与17.9 nmol NT等摩尔的剂量进行测试时,NT类似物[Gln4]NT、D-Trp11-NT和D-Arg8-NT具有细胞保护作用,而D-Arg9-NT则没有。促性腺激素释放激素(Gn-RH)和促黑素细胞激素释放抑制因子(MIF-1)这两种与NT结构不相关的寡肽在该模型中未表现出细胞保护功效。NT的C末端片段、异视蛋白和NT8 - 13以及N末端片段NT1 - 6完全无效。最后,NT的两个N末端片段NT1 - 8和NT1 - 10在该剂量水平下产生了显著的细胞保护活性。NT1 - 8和NT1 - 10提供的细胞保护作用与NT一样,呈剂量依赖性,其半数有效剂量(ED50)与NT相似(NT = 16.2 nmol,NT1 - 8 = 17.8 nmol,NT1 - 10 = 19.9 nmol)。总之,我们证明了被认为是NT降解产物的较小分子量形式的NT能够有效地发挥生物学作用。

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