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从负反馈中调节恢复脉冲式生长激素分泌:一项临床前研究。

Regulated recovery of pulsatile growth hormone secretion from negative feedback: a preclinical investigation.

机构信息

Endocrine Research Unit, Mayo School of Graduate Medical Education, Center for Translational Science Activities, Mayo Clinic, Rochester, MN 55905, USA.

出版信息

Am J Physiol Regul Integr Comp Physiol. 2011 Oct;301(4):R1143-52. doi: 10.1152/ajpregu.00293.2011. Epub 2011 Jul 27.

Abstract

Although stimulatory (feedforward) and inhibitory (feedback) dynamics jointly control neurohormone secretion, the factors that supervise feedback restraint are poorly understood. To parse the regulation of growth hormone (GH) escape from negative feedback, 25 healthy men and women were studied eight times each during an experimental GH feedback clamp. The clamp comprised combined bolus infusion of GH or saline and continuous stimulation by saline GH-releasing hormone (GHRH), GHRP-2, or both peptides after randomly ordered supplementation with placebo (both sexes) vs. E(2) (estrogen; women) and T (testosterone; men). Endpoints were GH pulsatility and entropy (a model-free measure of feedback quenching). Gender determined recovery of pulsatile GH secretion from negative feedback in all four secretagog regimens (0.003 ≤ P ≤ 0.017 for women>men). Peptidyl secretagog controlled the mass, number, and duration of feedback-inhibited GH secretory bursts (each, P < 0.001). E(2)/T administration potentiated both pulsatile (P = 0.006) and entropic (P < 0.001) modes of GH recovery. IGF-I positively predicted the escape of GH secretory burst number and mode (P = 0.022), whereas body mass index negatively forecast GH secretory burst number and mass (P = 0.005). The composite of gender, body mass index, E(2), IGF-I, and peptidyl secretagog strongly regulates the escape of pulsatile and entropic GH secretion from autonegative feedback. The ensemble factors identified in this preclinical investigation enlarge the dynamic model of GH control in humans.

摘要

虽然刺激(前馈)和抑制(反馈)动力学共同控制神经激素的分泌,但监督反馈抑制的因素知之甚少。为了分析生长激素(GH)逃避负反馈的调节,我们在一项实验性 GH 反馈钳夹中,对 25 名健康男性和女性进行了 8 次研究。钳夹包括 GH 或盐水的联合推注以及盐水 GH 释放激素(GHRH)、GHRP-2 或两者的连续刺激,之后按随机顺序给予安慰剂(男女)与 E2(雌激素;女性)和 T(睾酮;男性)。终点是 GH 脉冲性和熵(一种无模型反馈抑制的测量)。在所有四种激动剂方案中,性别决定了从负反馈中恢复脉冲性 GH 分泌(女性>男性,0.003≤P≤0.017)。肽激动剂控制反馈抑制的 GH 分泌爆发的数量、频率和持续时间(每个,P<0.001)。E2/T 给药增强了 GH 脉冲性和熵性恢复(P=0.006 和 P<0.001)。IGF-I 阳性预测 GH 分泌爆发数量和模式的逃逸(P=0.022),而体重指数负预测 GH 分泌爆发数量和质量(P=0.005)。性别、体重指数、E2、IGF-I 和肽激动剂的组合强烈调节了从自身负反馈中逃逸的脉冲性和熵性 GH 分泌。本临床前研究中确定的综合因素扩大了人类 GH 控制的动力学模型。

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