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通过输注生长激素释放激素拮抗剂可消除夜间生长激素(GH)分泌。

Nocturnal growth hormone (GH) secretion is eliminated by infusion of GH-releasing hormone antagonist.

作者信息

Ocampo-Lim B, Guo W, DeMott-Friberg R, Barkan A L, Jaffe C A

机构信息

Department of Internal Medicine, University of Michigan Medical Center, Ann Arbor 48109, USA.

出版信息

J Clin Endocrinol Metab. 1996 Dec;81(12):4396-9. doi: 10.1210/jcem.81.12.8954048.

Abstract

The neuroendocrine mechanisms underlying the generation of pulsatile GH secretion in humans are poorly understood. GH secretory pulses are likely to result from acute GHRH secretory episodes, acute decreases in hypothalamic somatostatin secretion, or a combination of these mechanisms. In earlier studies we demonstrated that a single i.v. bolus of a competitive GHRH antagonist [N-Ac-Tyr1,D-Arg2)GHRH-(1-29); GHRH-Ant] blocked 40% of the nocturnal GH release. Failure to more completely eliminate nocturnal GH secretion could be due to either incomplete antagonism of endogenous GHRH action by GHRH-Ant or a non-GHRH component of GH release. We subsequently investigated whether a continuous infusion of GHRH-Ant would more completely eliminate nocturnal GH secretion. Eight men were given a 400 micrograms/kg i.v. bolus of GHRH-Ant at 2300 h, followed by a 50 micrograms/kg.h i.v. infusion of GHRH-Ant between 2300-0700 h or a saline bolus followed by a saline infusion. An i.v. bolus of GHRH (1 microgram/kg) was given at 0500 h on both occasions. Blood was sampled every 10 min between 2300-0700 h. As measured by the area under the curve (AUC) from 2400-0500 h, GHRH-Ant suppressed GH secretion by an average of 89% (1795 +/- 412 vs. 164 +/- 46 micrograms/min.L; P = 0.004). The response to GHRH was suppressed by 79% (484 +/- 140 vs. 64 +/- 19 micrograms/min.L; P = 0.02). These data demonstrate that the previously observed nonsuppressible GH secretion was probably due to incomplete blockade of pituitary GHRH receptors and that all or nearly all of nocturnal GH pulsatility can be attributed to the effect of hypothalamic GHRH.

摘要

人类中脉冲式生长激素(GH)分泌产生的神经内分泌机制目前还知之甚少。GH分泌脉冲可能源于急性促生长激素释放激素(GHRH)分泌事件、下丘脑生长抑素分泌的急性减少,或这些机制的组合。在早期研究中,我们证明单次静脉注射竞争性GHRH拮抗剂[N - 乙酰 - 酪氨酸1,D - 精氨酸2)GHRH - (1 - 29);GHRH - Ant]可阻断40%的夜间GH释放。未能更完全消除夜间GH分泌可能是由于GHRH - Ant对内源性GHRH作用的拮抗不完全,或者是GH释放的非GHRH成分所致。我们随后研究了持续输注GHRH - Ant是否能更完全地消除夜间GH分泌。8名男性在23:00时静脉注射400微克/千克的GHRH - Ant推注,随后在23:00至07:00之间以50微克/千克·小时的速度静脉输注GHRH - Ant,或者先静脉注射生理盐水推注,随后输注生理盐水。在两种情况下,均在05:00时静脉注射1微克/千克的GHRH推注。在23:00至07:00之间每隔10分钟采集一次血液样本。通过24:00至05:00时的曲线下面积(AUC)测量,GHRH - Ant平均抑制GH分泌89%(1795±412对164±46微克/分钟·升;P = 0.004)。对GHRH的反应被抑制了79%(484±140对64±19微克/分钟·升;P = 0.02)。这些数据表明,先前观察到的不可抑制的GH分泌可能是由于垂体GHRH受体的阻断不完全,并且所有或几乎所有夜间GH脉冲都可归因于下丘脑GHRH的作用。

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