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24小时生长激素(GH)释放肽(GHRP)输注可增强GH的脉冲式分泌,并特异性减弱对随后一次GHRP推注的反应。

Twenty-four-hour growth hormone (GH)-releasing peptide (GHRP) infusion enhances pulsatile GH secretion and specifically attenuates the response to a subsequent GHRP bolus.

作者信息

Huhn W C, Hartman M L, Pezzoli S S, Thorner M O

机构信息

Department of Medicine, University of Virginia Health Sciences Center, Charlottesville 22908.

出版信息

J Clin Endocrinol Metab. 1993 May;76(5):1202-8. doi: 10.1210/jcem.76.5.8496311.

Abstract

GH-releasing peptide (GHRP; SK&F 110679) is a synthetic hexapeptide that specifically stimulates GH release through nonopiate non-GH-releasing hormone (non-GHRH) receptors. To determine the effects of a 24-h GHRP infusion, eight normal young men received infusions of saline for 2 h, then saline (on two occasions) or GHRP (1.0 micrograms/kg.h; on two occasions) for 24 h, followed by an iv bolus of GHRP or GHRH (1.0 micrograms/kg) and a 2.5-h saline infusion. Serum GH was measured every 10 min throughout the 28.5-h period. GH secretion rates [per L distribution volume (Lv)] were determined by deconvolution analysis; attributes of pulsatile GH release were assessed by Cluster analysis. GH secretion was enhanced and remained pulsatile during GHRP infusions. The two GHRP infusions increased GH secretion rates (micrograms per Lv/h) 8-fold compared to saline (GHRP, 12 +/- 2.1 and 12 +/- 2.2; saline, 1.5 +/- 0.34 and 1.4 +/- 0.27; P < 0.05). The number of GH pulses, pulse duration and height, incremental pulse amplitude, interpeak valley concentration, and individual pulse areas were significantly greater during GHRP infusions than during saline treatment. Attributes of pulsatile GH release on the two GHRP infusion days were significantly correlated, indicating that enhancement of GH secretion by GHRP is highly reproducible. Mean plasma insulin-like growth factor-I (IGF-I) concentrations increased 12% and 22% on GHRP infusion days, whereas IGF-I levels declined 18% and 20% during saline infusions (P < 0.05). GHRP infusion significantly attenuated the GH response to a subsequent GHRP bolus injection; both GH secretion rates (GHRP, 4.1 +/- 1.6; saline, 19 +/- 3.0 micrograms/Lv.h; P < 0.05) and peak GH concentrations (GHRP, 7.9 +/- 2.9; saline, 25 +/- 2.9 micrograms/L; P < 0.05) were decreased. In contrast, peak GH concentrations in response to GHRH were significantly increased after GHRP infusion compared to those after saline treatment (24 +/- 4.7 vs. 11 +/- 2.7 micrograms/L; P < 0.05). We conclude that 24-h GHRP infusions augment pulsatile GH release and increase plasma IGF-I concentrations without significant adverse effects. Attenuation of the GH response to a subsequent GHRP bolus is not caused by depletion of pituitary GH, since the response to a GHRH bolus was enhanced by prior infusion of GHRP.

摘要

生长激素释放肽(GHRP;SK&F 110679)是一种合成六肽,它通过非阿片类非生长激素释放激素(non-GHRH)受体特异性刺激生长激素释放。为了确定24小时输注GHRP的效果,8名正常年轻男性先接受2小时的生理盐水输注,然后接受24小时的生理盐水(两次)或GHRP(1.0微克/千克·小时;两次)输注,随后静脉推注GHRP或GHRH(1.0微克/千克)并进行2.5小时的生理盐水输注。在整个28.5小时期间,每10分钟测量一次血清生长激素。通过去卷积分析确定生长激素分泌率[每升分布容积(Lv)];通过聚类分析评估脉冲式生长激素释放的特征。在GHRP输注期间,生长激素分泌增强且仍保持脉冲式。与生理盐水相比,两次GHRP输注使生长激素分泌率(微克/Lv/小时)增加了8倍(GHRP,12±2.1和12±2.2;生理盐水,1.5±0.34和1.4±0.27;P<0.05)。在GHRP输注期间,生长激素脉冲数、脉冲持续时间和高度、增量脉冲幅度、峰间谷浓度以及单个脉冲面积均显著高于生理盐水治疗期间。两次GHRP输注日的脉冲式生长激素释放特征显著相关,表明GHRP对生长激素分泌的增强作用具有高度可重复性。在GHRP输注日,平均血浆胰岛素样生长因子-I(IGF-I)浓度分别增加了12%和22%,而在生理盐水输注期间,IGF-I水平分别下降了18%和20%(P<0.05)。GHRP输注显著减弱了随后推注GHRP时的生长激素反应;生长激素分泌率(GHRP,4.1±1.6;生理盐水,19±3.0微克/Lv/小时;P<0.05)和生长激素峰值浓度(GHRP,7.9±2.9;生理盐水,25±2.9微克/L;P<0.05)均降低。相反,与生理盐水治疗后相比,GHRP输注后对GHRH的生长激素峰值浓度显著增加(24±4.7对11±2.7微克/L;P<0.05)。我们得出结论,24小时输注GHRP可增强脉冲式生长激素释放并增加血浆IGF-I浓度,且无明显不良反应。对随后推注GHRP的生长激素反应减弱并非由垂体生长激素耗竭所致,因为之前输注GHRP可增强对推注GHRH的反应。

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