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Moderation of psychosocial risk factors through dysfunction of the hypothalamic-pituitary-adrenal stress axis in the onset of chronic widespread musculoskeletal pain: Findings of a population-based prospective cohort study

机译:通过慢性广泛性肌肉骨骼疼痛发作时下丘脑 - 垂体 - 肾上腺应力轴功能障碍缓解心理社会危险因素:基于人群的前瞻性队列研究的结果

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摘要

Objective. To test the hypothesis that abnormalities in the hypothalamic-pituitary-adrenal (HPA) stress-response system would act as an effect moderator between HPA function and the onset of chronic widespread pain (CWP). Methods. We conducted a population-based prospective cohort study. Current pain and psychosocial status were ascertained in 11,000 subjects. Of the 768 eligible subjects free of CWP but at future risk based on their psychosocial profile, 463 were randomly selected, and 267 (57.7%) consented to assessment of their HPA axis function. Diurnal function was measured by assessing levels of salivary cortisol in the morning (9:00 AM) and evening (10:00 PM). Serum cortisol levels were measured after an overnight low-dose (0.25 mg) dexamethasone suppression test and a potentially stressful clinical examination. All subjects were followed up 15 months later to identify cases of new-onset CWP. Results. A total of 241 subjects (94.9%) completed the followup study, and 28 (11.6%) reported the new onset of CWP. High levels of cortisol post-dexamethasone (odds ratio [OR] 3.53, 95% confidence interval [95% CI] 1.17-10.65), low levels in morning saliva (OR 1.43, 95% CI 0.52-3.94), and high levels in evening saliva (OR 2.32, 95% CI 0.64-8.42) were all associated with CWP. These 3 factors were found to be independent and additive predictors of CWP (OR for all 3 factors 8.5, 95% CI 1.5-47.9) in analyses controlling for age, sex, depression, sleep disturbance, recent traumatic life events, and pain status. One or more of these 3 HPA factors identified 26 (92.9%) cases of new-onset CWP. Conclusion. Among a group of psychologically at-risk subjects, dysfunction of the HPA axis helps to distinguish those who will and will not develop new-onset CWP. © 2007, American College of Rheumatology.
机译:目的。为了检验关于下丘脑-垂体-肾上腺(HPA)应激反应系统异常的假设,可以作为HPA功能与慢性广泛性疼痛(CWP)发作之间的效应调节剂。方法。我们进行了一项基于人群的前瞻性队列研究。在11,000名受试者中确定了当前的疼痛和社会心理状况。在768名无CWP但根据其心理社会状况处于未来风险中的合格受试者中,随机选择了463名,并且267名(57.7%)同意评估其HPA轴功能。通过评估上午(9:00 AM)和晚上(10:00 PM)唾液皮质醇的水平来测定昼夜功能。在过夜低剂量(0.25 mg)地塞米松抑制试验和可能产生压力的临床检查后,测量血清皮质醇水平。 15个月后对所有受试者进行了随访,以发现新发的CWP病例。结果。共有241名受试者(94.9%)完成了随访研究,其中28名(11.6%)报告了新的CWP发作。地塞米松后皮质醇水平高(比值[OR] 3.53,95%置信区间[95%CI] 1.17-10.65),早晨唾液水平低(OR 1.43,95%CI 0.52-3.94),高唾液酸水平夜间唾液(OR 2.32,95%CI 0.64-8.42)均与CWP相关。在控制年龄,性别,抑郁,睡眠障碍,近期创伤性生活事件和疼痛状态的分析中,发现这3个因素是CWP的独立预测因子和CWP的附加预测因子(所有3个因子均为8.5,95%CI 1.5-47.9)。这3个HPA因子中的一个或多个确定了26例(92.9%)新发CWP病例。结论。在一组有心理风险的受试者中,HPA轴功能障碍有助于区分那些会和不会发展新发作的CWP的人。 ©2007,美国风湿病学院。

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