Peino R, Cordido F, Peñalva A, Alvarez C V, Dieguez C, Casanueva F F
Department of Medicine, School of Medicine, Santiago de Compostela University, Spain.
J Clin Endocrinol Metab. 1996 Mar;81(3):909-13. doi: 10.1210/jcem.81.3.8772549.
Increases in plasma free fatty acids (FFA) inhibit the GH response to a variety of stimuli; however, the role of FFA depression in GH control is far from understood. In the present work, FFA reduction was obtained by the administration to normal subjects of acipimox, a lipid-lowering drug devoid of side-effects. Each subject tested underwent two paired tests. In one, acipimox was administered orally at a dose of 250 mg at -270 min and at a dose of 250 mg at -60 min; in the matched test, placebo was given at similar intervals. To induce GH release, four stimuli acting through different mechanisms were used: pyridostigmine (120 mg, orally) at -60 min, GHRH (1 microgram/kg, iv) at 0 min, GH-releasing peptide (GHRP-6; His-D-Trp-Ala-Trp-D-Phe-Lys-NH2; 1 microgram/kg, iv) at 0 min, and finally, GHRH plus GHRP-6 at the same doses at 0 min. GH secretion was analyzed as the area under the secretory curve (AUC; mean +/- SE, micrograms per L/120 min). Acipimox pretreatment alone (n = 6) induced a reduction in FFA levels compared with placebo treatment. The FFA reduction led to a sustained GH secretion that increased from 2.4 +/- 1.8 micrograms/L at -120 min to 14.2 +/- 4.0 at 120 min. The GH AUC for placebo was 266 +/- 100, and that for acipimox was 1781 +/- 408 (P < 0.05). In the pyridostigmine-treated group (n = 6), the acipimox-pyridostigmine AUC (2046 +/- 323) was higher (P < 0.05) than the placebo-pyridostigmine AUC (764 +/- 101), but was not different from the AUC of acipimox alone. Previous FFA reduction nearly doubled the GHRH-mediated GH secretion (n = 6; placebo-GHRH AUC, 1817 +/- 365; acipimox-GHRH test, 3228 +/- 876; P < 0.05). A similar enhancement was observed when the stimulus employed was GHRP-6 (n = 6; placebo-GHRP-6 AUC, 2034 +/- 295; acipimox-GHRP-6, 4827 +/- 703; P < 0.05). Furthermore, even the most potent GH stimulus known to date, i.e. GHRH plus GHRP-6, was enhanced by the FFA suppression (placebo-GHRH-GHRP-6 AUC, 2034 +/- 277; acipimox-GHRH-GHRP-6, 5809 +/- 758; P < 0.05). The enhancing effect of lowering FFA levels was additive regardless of the stimulus employed. These results indicate that 1) FFA reduction per se stimulates GH secretion with a delayed time of action; 2) FFA reduction enhanced in an additive manner the GH secretion elicited by such different stimuli as pyridostigmine, GHRH, and GHRP-6; and 3) the observation that FFA reduction enhanced the response to the most potent GH stimulus, GHRH plus GHRP-6, suggests that FFA suppression acts by a separate mechanism. FFA reduction may have value in the clinical setting for assessing GH reserve.
血浆游离脂肪酸(FFA)水平升高会抑制生长激素(GH)对多种刺激的反应;然而,FFA水平降低在GH调控中的作用仍远未明确。在本研究中,通过给正常受试者服用阿西莫司(一种无副作用的降脂药物)来降低FFA水平。每个受试对象都进行了两组配对试验。一组试验中,在 -270分钟时口服250毫克阿西莫司,在 -60分钟时再口服250毫克;在配对试验中,在相似的时间间隔给予安慰剂。为诱导GH释放,使用了四种通过不同机制起作用的刺激物:在 -60分钟时口服吡啶斯的明(120毫克),在0分钟时静脉注射生长激素释放激素(GHRH,1微克/千克),在0分钟时静脉注射生长激素释放肽(GHRP - 6;His - D - Trp - Ala - Trp - D - Phe - Lys - NH2;1微克/千克),最后,在0分钟时以相同剂量同时静脉注射GHRH和GHRP - 6。GH分泌以分泌曲线下面积(AUC;平均值±标准误,微克每升/120分钟)进行分析。与安慰剂治疗相比,单独使用阿西莫司预处理(n = 6)可使FFA水平降低。FFA水平降低导致GH分泌持续增加,从 -120分钟时的2.4±1.8微克/升增加到120分钟时的14.2±4.0微克/升。安慰剂组的GH AUC为266±100,阿西莫司组为1781±408(P < 0.05)。在吡啶斯的明治疗组(n = 6)中,阿西莫司 - 吡啶斯的明AUC(2046±323)高于安慰剂 - 吡啶斯的明AUC(764±101)(P < 0.05),但与单独使用阿西莫司的AUC无差异。预先降低FFA水平使GHRH介导的GH分泌增加了近一倍(n = 6;安慰剂 - GHRH AUC,1817±365;阿西莫司 - GHRH试验,3228±876;P < 0.05)。当刺激物为GHRP - 6时也观察到了类似的增强作用(n = 6;安慰剂 - GHRP - 6 AUC,2034±295;阿西莫司 - GHRP - 6,4827±703;P < 0.05)。此外,即使是迄今为止已知的最有效的GH刺激物,即GHRH加GHRP - 6,也因FFA抑制而增强(安慰剂 - GHRH - GHRP - 6 AUC,2034±277;阿西莫司 - GHRH - GHRP - 6,5809±758;P < 0.05)。无论使用何种刺激物,降低FFA水平的增强作用都是相加的。这些结果表明:1)FFA水平降低本身可刺激GH分泌,且作用时间延迟;2)FFA水平降低以相加的方式增强了由吡啶斯的明、GHRH和GHRP - 6等不同刺激物引发的GH分泌;3)FFA水平降低增强了对最有效的GH刺激物GHRH加GHRP - 6的反应,这一观察结果表明FFA抑制通过一种独立的机制起作用。降低FFA水平在临床评估GH储备方面可能具有价值。
