Iranmanesh A, South S, Liem A Y, Clemmons D, Thorner M O, Weltman A, Veldhuis J D
Medical Service, Veterans Affairs Medical Center, Salem, Virginia 24153, USA.
Eur J Endocrinol. 1998 Jul;139(1):59-71. doi: 10.1530/eje.0.1390059.
We here investigate the potential rescue of the relative hyposomatotropism of aging and obesity by 3-day pulsatile GHRH infusions (i.v. bolus 0.33 microg/kg every 90 min) in 19 healthy men of varying ages (18 to 66 years) and body compositions (12 to 37% total body fat). Baseline (control) and GHRH-driven pulsatile GH secretion (in randomly ordered sessions) were quantitated by deconvolution analysis of 24-h (10-min sampling) serum GH concentration profiles measured in an ultrasensitive (threshold 0.005 microg/l) chemiluminescence assay. GHRH infusion significantly increased the mean (24-h) serum GH concentration (0.3 +/- 0.1 basal vs 2.4 +/- 0.4 microg/l treatment; P = 0.0001), total daily pulsatile GH production rate (21 +/- 9.5 vs 97 +/- 17 microg/l/day; P = 0.01), GH secretory burst frequency (11 +/- 0.5 vs 17 +/- 0.3 events/day; P = <0.01), and mass of GH released per burst (1.1 +/- 0.4 vs 5.9 1 microg/l; P < 0.01), as well as serum IGF-I (261 +/- 33 vs 436 +/- 37 microg/l; P = 0.005), insulin (45 +/- 13 vs 79 +/- 17 mU/l; P = 0.0002), and IGF binding protein (IGFBP)-3 (3320 +/- 107 vs 4320 +/- 114 microg/l; P = 0.001) concentrations, while decreasing IGFBP-1 levels (16 +/- 1.2 vs 14 +/- 0.09 microg/l; P = 0.02). Serum total testosterone and estradiol concentrations did not change. GHRH treatment also reduced the half-duration of GH secretory bursts, and increased the GH half-life. GHRH-stimulated 24-h serum GH concentrations and the mass of GH secreted per burst were correlated negatively with age (R[value]:P[value] = -0.67:0.002 and -0.58:0.009 respectively), and percentage body fat (R:P = -0.80:0.0001 and -0.65:0.0005 respectively), but positively with serum testosterone concentrations (R:P = +0.55:0.016 and +0.53:0.019 respectively). GHRH-stimulated plasma IGF-I increments correlated negatively with age and body mass index, and positively with serum testosterone, but not with percentage body fat. Cosinor analysis disclosed persistent nyctohemeral rhythmicity of GH secretory burst mass (with significantly increased 24-h amplitude and mesor values) but unchanged acrophase during fixed pulsatile GHRH infusions, which suggests that both GHRH- and non-GHRH-dependent mechanisms can modulate the magnitude (but only non-GHRH mechanisms can modulate the timing) of somatotrope secretory activity differentially over a 24-h period. In summary, diminished GHRH action and/or non-GHRH-dependent mechanisms (e.g. somatostatin excess, putative endogenous growth hormone-releasing peptide deficiency etc.) probably underlie the hyposomatotropism of aging, (relative) obesity, and/or hypoandrogenemia. Preserved or increased tissue IGF-I responses to GHRH-stimulated GH secretion (albeit absolutely reduced, suggesting GHRH insensitivity in obesity) may distinguish the pathophysiology of adiposity-associated hyposomatotropism from that of healthy aging.
我们在此研究了在19名年龄各异(18至66岁)、身体组成不同(体脂率12%至37%)的健康男性中,通过3天的脉冲式生长激素释放激素(GHRH)静脉输注(每90分钟静脉推注0.33微克/千克)来挽救衰老和肥胖相关的相对生长激素分泌不足的可能性。通过对超敏(检测阈值0.005微克/升)化学发光法测定的24小时(每10分钟采样)血清生长激素浓度曲线进行反卷积分析,对基线(对照)和GHRH驱动的脉冲式生长激素分泌(在随机安排的实验时段)进行定量。GHRH输注显著提高了平均(24小时)血清生长激素浓度(基础值0.3±0.1微克/升,治疗值2.4±0.4微克/升;P = 0.0001)、每日总脉冲式生长激素产生率(21±9.5微克/升/天,治疗值97±17微克/升/天;P = 0.01)、生长激素分泌脉冲频率(11±0.5次/天,治疗值17±0.3次/天;P < 0.01)以及每次脉冲释放的生长激素量(1.1±0.4微克/升,治疗值5.9±1微克/升;P < 0.01),同时提高了血清胰岛素样生长因子-I(IGF-I)(261±33微克/升,治疗值436±37微克/升;P = 0.005)、胰岛素(45±13毫单位/升,治疗值7
