接受氢化可的松治疗的患者,血清皮质醇和糖皮质激素代谢物对骨骼健康的不良影响。
The contribution of serum cortisone and glucocorticoid metabolites to detrimental bone health in patients receiving hydrocortisone therapy.
机构信息
Department of Endocrinology, Tallaght University Hospital, Dublin, Ireland.
Academic Department of Endocrinology, Beaumont Hospital and Royal College of Surgeons in Ireland, Dublin, Ireland.
出版信息
BMC Endocr Disord. 2020 Oct 10;20(1):154. doi: 10.1186/s12902-020-00633-1.
BACKGROUND
Glucocorticoid therapy is the most common cause of iatrogenic osteoporosis. Less is known regarding the effect of glucocorticoids when used as replacement therapy on bone remodelling in patients with adrenal insufficiency. Enhanced intracellular conversion of inactive cortisone to active cortisol, by 11 beta-hydroxysteroid dehydrogenase type 1(11β-HSD1) and other enzymes leading to alterations in glucocorticoid metabolism, may contribute to a deleterious effect on bone health in this patient group.
METHODS
Study design: An open crossover prospective study randomizing ten hypopituitary men, with severe ACTH deficiency, to three commonly used hydrocortisone dose regimens.
MEASUREMENTS
Following 6 weeks of each regimen, patients underwent 24-h serum cortisol/cortisone sampling, measurement of bone turnover markers, and a 24-h urine collection for measurement of urinary steroid metabolites by gas chromatography-mass spectrometry (GC-MS). Serum cortisone and cortisol were analysed by liquid chromatography-mass spectrometry (LC-MS).
RESULTS
Dose-related and circadian variations in serum cortisone were seen to parallel those for cortisol, indicating conversion of ingested hydrocortisone to cortisone. The median area under the curve (AUC) of serum cortisone was significantly higher in patients on dose A (20 mg/10 mg) [670.5 (IQR 621-809.2)] compared to those on dose C (10 mg/5 mg) [562.8 (IQR 520.1-619.6), p = 0.01]. A negative correlation was observed between serum cortisone and bone formation markers, OC [1-49] (r = - 0.42, p = 0.03), and PINP (r = - 0.49, p = 0.01). There was a negative correlation between the AUC of night-time serum cortisone levels with the bone formation marker, OC [1-49] (r = - 0.41, p = 0.03) but there were no significant correlations between day-time serum cortisone or cortisol with bone turnover markers. There was a negative correlation between total urinary cortisol metabolites and the bone formation markers, PINP (r = - 0.39, p = 0.04), and OC [1-49] (r = - 0.35, p = 0.06).
CONCLUSION
Serum cortisol and cortisone and total urinary corticosteroid metabolites are negatively associated with bone turnover markers in patients receiving replacement doses of hydrocortisone, with nocturnal glucocorticoid exposure having a potentially greater influence on bone turnover.
TRIAL REGISTRATION
Irish Medicines Board Clinical Trial Number - CT900/459/1 and EudraCT Number - 2007-005018-37 . Registration date: 07-09-2007.
背景
糖皮质激素治疗是医源性骨质疏松症最常见的原因。对于肾上腺功能不全患者使用糖皮质激素作为替代治疗对骨重塑的影响,人们知之甚少。11β-羟甾类脱氢酶 1(11β-HSD1)和其他酶增强了无活性可的松向活性皮质醇的细胞内转化,导致糖皮质激素代谢的改变,这可能对这群患者的骨骼健康产生有害影响。
方法
研究设计:一项开放交叉前瞻性研究,将 10 名严重 ACTH 缺乏的垂体功能减退男性患者随机分为三组,接受三种常用的氢化可的松剂量方案。
测量
在每个方案 6 周后,患者接受 24 小时血清皮质醇/皮质酮采样、骨转换标志物测量和 24 小时尿液收集,通过气相色谱-质谱法(GC-MS)测量尿甾体代谢物。用液相色谱-质谱法(LC-MS)分析血清皮质酮和皮质醇。
结果
观察到血清皮质酮的剂量相关性和昼夜变化与皮质醇的变化平行,表明摄入的氢化可的松转化为皮质酮。接受剂量 A(20mg/10mg)[670.5(IQR 621-809.2)]的患者的血清皮质酮中位 AUC 明显高于接受剂量 C(10mg/5mg)[562.8(IQR 520.1-619.6),p=0.01]。血清皮质酮与骨形成标志物 OC[1-49](r=-0.42,p=0.03)和 PINP(r=-0.49,p=0.01)呈负相关。夜间血清皮质酮水平的 AUC 与骨形成标志物 OC[1-49](r=-0.41,p=0.03)呈负相关,但白天血清皮质醇或皮质酮与骨转换标志物无显著相关性。总尿皮质类固醇代谢物与骨形成标志物 PINP(r=-0.39,p=0.04)和 OC[1-49](r=-0.35,p=0.06)呈负相关。
结论
接受氢化可的松替代剂量的患者中,血清皮质醇和皮质酮以及总尿皮质类固醇代谢物与骨转换标志物呈负相关,夜间糖皮质激素暴露对骨转换的影响可能更大。
试验注册
爱尔兰药品管理局临床试验编号 - CT900/459/1 和 EudraCT 编号 - 2007-005018-37。注册日期:2007 年 9 月 7 日。
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