Roelfsema Ferdinand, Aoun Paul, Takahashi Paul Y, Erickson Dana, Yang Rebecca, Veldhuis Johannes D
Department of Endocrinology and Metabolism, Leiden University Medical Center, 2333ZA Leiden, The Netherlands.
Endocrine Research Unit, Mayo School of Graduate Medical Education, Center for Translational Science Activities, Mayo Clinic, Rochester, Minnesota 55902.
J Clin Endocrinol Metab. 2017 Jul 1;102(7):2611-2619. doi: 10.1210/jc.2017-00115.
Adrenocorticotropic hormone (ACTH) secretion is controlled by unobservable hypothalamic corticotropin-releasing hormone (CRH) and arginine vasopressin (AVP) pulses. Clamping exogenous CRH or AVP input could allow indirect quantification of the impact of the endogenous heterotypic hormone.
We conducted a randomized, double-blind, placebo-controlled, crossover study in 28 healthy adults (16 men). Volunteers underwent a sex-steroid clamp and a cortisol clamp. ACTH was measured over 10 hours by 10-minute sampling during each of four randomized intravenous (IV) secretagogue clamps (i.e., continuous IV CRH, AVP, both peptides, or saline). Desensitization was tested by bolus injection of the noninfused peptide.
Mean ± standard error of the mean 10-hour ACTH concentrations (ng/L) in the sex-combined analysis were: saline, 32 ± 4.6; AVP, 29 ± 4.6; CRH, 67 ± 6.2; and CRH-AVP, 67 ± 8.8 (any CRH vs AVP or saline, P < 0.0001). CRH and AVP increased approximate entropy (relative randomness) of ACTH release (P < 0.0001). Bolus AVP injection after CRH infusion yielded a 2.5-hour ACTH concentration of 46 ± 4.3, exceeding that seen after bolus CRH or saline injection (26 ± 3.3 and 24 ± 3.6, respectively; P = 0.002 and 0.001). Sex hormone clamps did not influence ACTH levels.
A CRH, but not AVP, clamp yields sustained pulsatile ACTH secretion with high ACTH secretory-burst mass and randomness. After 10-hour CRH infusion, bolus AVP but not CRH, evoked marked ACTH release, likely caused by heterotypic sensitization of corticotropes by CRH. Similar interactions might underlie chronic stress states.
促肾上腺皮质激素(ACTH)的分泌受难以观察到的下丘脑促肾上腺皮质激素释放激素(CRH)和精氨酸加压素(AVP)脉冲的控制。钳制外源性CRH或AVP输入可间接量化内源性异型激素的影响。
我们对28名健康成年人(16名男性)进行了一项随机、双盲、安慰剂对照的交叉研究。志愿者接受了性类固醇钳制和皮质醇钳制。在四次随机静脉注射(IV)促分泌素钳制(即持续静脉注射CRH、AVP、两种肽或生理盐水)期间,通过每10分钟采样一次,在10小时内测量ACTH。通过推注未输注的肽来测试脱敏情况。
在性别综合分析中,10小时ACTH浓度(ng/L)的平均值±平均标准误差为:生理盐水组,32±4.6;AVP组,29±4.6;CRH组,67±6.2;CRH-AVP组,67±8.8(任何CRH组与AVP组或生理盐水组相比,P<0.0001)。CRH和AVP增加了ACTH释放的近似熵(相对随机性)(P<0.0001)。CRH输注后推注AVP产生的2.5小时ACTH浓度为46±4.3,超过了推注CRH或生理盐水后观察到的浓度(分别为26±3.3和24±3.6;P=0.002和0.001)。性激素钳制不影响ACTH水平。
CRH钳制而非AVP钳制可产生持续的脉动性ACTH分泌,具有高ACTH分泌爆发量和随机性。在10小时CRH输注后,推注AVP而非CRH可引起明显的ACTH释放,这可能是由于CRH对促肾上腺皮质细胞的异型致敏所致。类似的相互作用可能是慢性应激状态的基础。