Bergendahl M, Iranmanesh A, Mulligan T, Veldhuis J D
Department of Pediatrics, University of Turku, Finland.
J Clin Endocrinol Metab. 2000 Jun;85(6):2203-14. doi: 10.1210/jcem.85.6.6628.
The present study tests the clinical hypothesis that aging impairs homeostatic adaptations of cortisol secretion to stress. To this end, we implemented a short-term 3.5-day fast as an ethically acceptable metabolic stressor in eight young (ages 18-35 yr) and eight older (ages 60-72 yr) healthy men. Volunteers were studied in randomly ordered fed vs. fasting sessions. To capture the more complex dynamics of cortisol's feedback control, blood was sampled every 10 min for 24 h for later RIA of serum cortisol concentrations and quantitation of the pulsatile, entropic, and 24-h rhythmic modes of cortisol release using deconvolution analysis, the approximate entropy statistic, and cosine regression, respectively. The stress of fasting elevated the mean (24-h) serum cortisol concentration equivalently in the two age cohorts [i.e. from 7.2 +/- 0.35 to 11.6 +/- 0.71 microg/dL in young men and from 7.7 +/- 0.39 to 12.6 +/- 0.59 microg/dL in older individuals (P < 10(-7))]. The rise in integrated cortisol output was driven mechanistically by selective augmentation of cortisol secretory burst mass (P = 0.002). The resultant daily (pulsatile) cortisol secretion rate increased significantly but equally in young (from 94 +/- 6.3 to 151 +/- 15 microg/dL x day) and older (from 85 +/- 5.4 to 145 +/- 7.3 microg/dL x day) volunteers (P < 10(-4)). Nutrient restriction also prompted a marked reduction in the quantifiable regularity of (univariate) cortisol release patterns in both cohorts (P < 10(-4)). However, older men showed loss of joint synchrony of cortisol and LH secretion even in the fed state, which failed to change with metabolic stress (P < 10(-6)). In addition, older individuals maintained a premature (early-day) cortisol elevation in the fed state and unexpectedly evolved an anomalous further cortisol phase advance of 99 +/- 16 min during fasting (P < 10(-5)). Caloric deprivation in aging men also disproportionately elevated the mesor of 24-h rhythmic cortisol release (P = 10(-7)) and elicited a greater increment in the mean day-night variation in cortisol secretory-burst mass (P < 0.01 vs. young controls). Lastly, short-term caloric depletion in older subjects paradoxically normalized their age-associated suppression of the 24-h rhythm in cortisol interburst intervals. In summary, acute metabolic stress in healthy aging men (compared with young individuals) unmasks distinct, albeit complex, disruption of cortisol homeostasis. These dynamic anomalies impact the feedback-dependent and time-sensitive coupling of pulsatile and 24-h rhythmic cortisol secretion. Nutrient-withdrawal stress in the older male heightens the cortisol phase disparity already evident in fed elderly individuals. Conversely, the stress of fasting in young men paradoxically reproduces selected features of the aging unstressed (fed) cortisol axis; viz., abrogation of joint cortisol-LH synchrony and suppression of the normal diurnal variation in cortisol burst frequency. Whether fasting would unveil analogous disruption of feedback-dependent control of the corticotropic axis in healthy aging women is not yet known.
本研究检验了衰老会损害皮质醇分泌对压力的稳态适应这一临床假设。为此,我们在8名年轻(18 - 35岁)和8名年长(60 - 72岁)健康男性中实施了为期3.5天的短期禁食,作为一种符合伦理的代谢应激源。志愿者在随机安排的进食与禁食阶段接受研究。为了捕捉皮质醇反馈控制更复杂的动态变化,每10分钟采集一次血样,持续24小时,随后对血清皮质醇浓度进行放射免疫分析,并分别使用反卷积分析、近似熵统计和余弦回归对皮质醇释放的脉冲式、熵式和24小时节律模式进行定量分析。禁食应激使两个年龄组的平均(24小时)血清皮质醇浓度同等升高[即年轻男性从7.2±0.35微克/分升升至11.6±0.71微克/分升,年长个体从7.7±0.39微克/分升升至12.6±0.59微克/分升(P < 10⁻⁷)]。皮质醇综合输出量的增加在机制上是由皮质醇分泌脉冲量的选择性增加驱动的(P = 0.002)。由此产生的每日(脉冲式)皮质醇分泌率在年轻志愿者(从94±6.3微克/分升·天升至151±15微克/分升·天)和年长志愿者(从85±5.4微克/分升·天升至145±7.3微克/分升·天)中均显著增加且增加幅度相同(P < 10⁻⁴)。营养限制还促使两个年龄组中(单变量)皮质醇释放模式的可量化规律性显著降低(P < 10⁻⁴)。然而,年长男性即使在进食状态下也表现出皮质醇和促黄体生成素分泌的联合同步性丧失,且这种情况在代谢应激下并未改变(P < 10⁻⁶)。此外,年长个体在进食状态下维持着过早(日间早期)的皮质醇升高,并且在禁食期间意外地出现了99±16分钟的异常皮质醇相位提前(P < 10⁻⁵)。老年男性的热量剥夺还使24小时节律性皮质醇释放的中值显著升高(P = 10⁻⁷),并导致皮质醇分泌脉冲量的日夜平均变化有更大幅度的增加(与年轻对照组相比,P < 0.01)。最后,老年受试者的短期热量消耗反常地使他们与年龄相关的皮质醇脉冲间期24小时节律抑制恢复正常。总之,健康老年男性(与年轻个体相比)的急性代谢应激揭示了皮质醇稳态的明显但复杂的破坏。这些动态异常影响了脉冲式和24小时节律性皮质醇分泌的反馈依赖性和时间敏感性耦合。老年男性的营养剥夺应激加剧了进食状态下老年个体中已经明显的皮质醇相位差异。相反,年轻男性的禁食应激反常地重现了未受应激(进食)的老年皮质醇轴的某些特征;即,皮质醇 - 促黄体生成素联合同步性的废除和皮质醇脉冲频率正常昼夜变化的抑制。尚不清楚禁食是否会揭示健康老年女性促肾上腺皮质激素轴反馈依赖性控制的类似破坏。
