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人肾上腺髓质素13 - 52与大鼠和仓鼠微血管中降钙素基因相关肽受体的相互作用。

Interaction of human adrenomedullin 13-52 with calcitonin gene-related peptide receptors in the microvasculature of the rat and hamster.

作者信息

Hall J M, Siney L, Lippton H, Hyman A, Kang-Chang J, Brain S D

机构信息

Biomedical Sciences Division, King's College London, U.K.

出版信息

Br J Pharmacol. 1995 Feb;114(3):592-7. doi: 10.1111/j.1476-5381.1995.tb17180.x.

Abstract
  1. Adrenomedullin (ADM), a recently discovered circulating hypotensive peptide, shares limited sequence homology with the sensory nerve-derived vasodilator, calcitonin gene-related peptide (CGRP). This study compared the vasodilator effect of sequence 13-52 of human adrenomedullin (ADM13-52) with that of human alpha CGRP (CGRP), in the microvasculature of the hamster cheek pouch and rat skin in vivo. 2. Single arterioles (20-40 microns diameter) in the hamster cheek pouch were visualised by intravital microscopy and video recording, and measured by image analysis. Both ADM13-52 (1 pmol-0.4 nmol) and CGRP (0.1 pmol-1 nmol) evoked dose-related increases in the diameter of preconstricted arterioles (n = 6). ADM13-52 (ED50 14 pmol) was 20 fold less active than CGRP (ED50 0.71 pmol). The kinetics of onset and decline of vasodilator responses to both peptides were similar, with vasodilator responses to both peptides reaching a maximum at ca. 2 min, and reversing after 10-15 min (n = 5-7). The submaximal increase in blood flow evoked by ADM13-52 was significantly inhibited (P < 0.05; n = 6) by the CGRP1 receptor antagonist, CGRP8-37, at a dose (300 nmol kg-1, i.v.) that we have previously shown to inhibit significantly equivalent vasodilator responses to CGRP in this preparation. 3. In experiments measuring changes in local blood flow in rat skin by a 133xenon clearance technique, intradermal injection of both ADM13-52 (3-300 pmol) and CGRP (0.1-30 pmol) evoked dose-related increases in local blood flow. ADM13-52 (ED50 27 pmol) was 17 fold less potent than CGRP (ED501.6 pmol) (n = 6). The submaximal increase in blood flow evoked by both peptides was significantly inhibited (P<0.02; n = 5) by CGRP837 (100 nmol kg-1, i.v.).4. We conclude that ADM13-52 is a potent vasodilator in the microvasculature of the hamster and rat invivo. It mediates its vasodilator effect by arteriolar dilatation and this effect is due, at least in part, to the stimulation of CGRPI receptors.
摘要
  1. 肾上腺髓质素(ADM)是一种最近发现的循环性降压肽,与感觉神经源的血管舒张剂降钙素基因相关肽(CGRP)的序列同源性有限。本研究在仓鼠颊囊和大鼠皮肤的体内微循环中,比较了人肾上腺髓质素13 - 52序列(ADM13 - 52)与人αCGRP(CGRP)的血管舒张作用。2. 通过活体显微镜和视频记录观察仓鼠颊囊中直径为20 - 40微米的单个小动脉,并通过图像分析进行测量。ADM13 - 52(1皮摩尔 - 0.4纳摩尔)和CGRP(0.1皮摩尔 - 1纳摩尔)均可引起预收缩小动脉直径的剂量相关性增加(n = 6)。ADM13 - 52(半数有效剂量14皮摩尔)的活性比CGRP(半数有效剂量0.71皮摩尔)低20倍。两种肽引起的血管舒张反应的起始和消退动力学相似,两种肽的血管舒张反应在约2分钟时达到最大值,并在10 - 15分钟后恢复(n = 5 - 7)。CGRP1受体拮抗剂CGRP8 - 37(静脉注射剂量300纳摩尔/千克)可显著抑制(P < 0.05;n = 6)ADM13 - 52引起的次最大血流增加,我们之前已证明该剂量可显著抑制本制剂中对CGRP的等效血管舒张反应。3. 在通过133氙清除技术测量大鼠皮肤局部血流变化的实验中,皮内注射ADM13 - 52(3 - 300皮摩尔)和CGRP(0.1 - 30皮摩尔)均可引起局部血流的剂量相关性增加。ADM13 - 52(半数有效剂量27皮摩尔)的效力比CGRP(半数有效剂量1.6皮摩尔)低17倍(n = 6)。CGRP837(静脉注射100纳摩尔/千克)可显著抑制(P < 0.02;n = 5)两种肽引起的次最大血流增加。4. 我们得出结论,ADM13 - 52在仓鼠和大鼠的体内微循环中是一种有效的血管舒张剂。它通过小动脉扩张介导其血管舒张作用,并且这种作用至少部分是由于对CGRP1受体的刺激。

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