慢性炎症性疾病儿童和成人使用口服糖皮质激素与骨坏死:一项基于人群的队列研究。
Oral glucocorticoid use and osteonecrosis in children and adults with chronic inflammatory diseases: a population-based cohort study.
作者信息
Horton Daniel B, Haynes Kevin, Denburg Michelle R, Thacker Mihir M, Rose Carlos D, Putt Mary E, Leonard Mary B, Strom Brian L
机构信息
Department of Pediatrics, Rutgers Robert Wood Johnson Medical School, Rutgers Center for Pharmacoepidemiology and Treatment Science, Institute for Health, Health Care Policy and Aging Research, Rutgers School of Public Health, Rutgers Biomedical and Health Sciences, New Brunswick, New Jersey, USA.
HealthCore, Wilmington, Delaware, USA.
出版信息
BMJ Open. 2017 Jul 21;7(7):e016788. doi: 10.1136/bmjopen-2017-016788.
OBJECTIVES
We studied oral glucocorticoids and osteonecrosis, a rare but serious bone disease, in individuals with various chronic inflammatory diseases. We hypothesised that we would find stronger associations in adults versus children and in people with autoimmune diseases.
DESIGN
Retrospective cohort study.
SETTING
Population-representative data (1994-2013) from general practices in the UK.
PARTICIPANTS
Children and adults diagnosed with asthma; inflammatory bowel disease; juvenile, psoriatic or rheumatoid arthritis; psoriasis; or systemic lupus.
EXPOSURES
Oral glucocorticoid patterns.
PRIMARY AND SECONDARY OUTCOME MEASURES
Diagnosed osteonecrosis (primary) and osteonecrosis plus clinical features (eg, symptoms, pain medication, surgical repair) (secondary). Discrete time failure models estimated the adjusted hazard ratio (aHR) of incident osteonecrosis following oral glucocorticoid exposure. Hypothesis testing was one sided (with corresponding 90% CI) since glucocorticoids were unlikely protective.
RESULTS
After adjusting for demographic, disease-related and health utilisation factors, glucocorticoid exposure was associated with osteonecrosis in adults (ages 18-49, aHR 2.1 (90% CI 1.5 to 2.9); ages ≥50, aHR 1.3 (90% CI 1.01 to 1.7)). However, low-dose glucocorticoids, corresponding to average doses <7.5 mg prednisolone daily and maximum doses <30 mg daily, were not associated with osteonecrosis in adults. Furthermore, even at high glucocorticoid doses, there was no evidence of increased osteonecrosis among glucocorticoid-exposed children (p=0.04 for interaction by age) (any glucocorticoid exposure, ages 2-9: aHR 1.1 (90% CI 0.7 to 1.7); ages 10-17: aHR 0.6 (90% CI 0.3 to 1.6)). Arthritis, inflammatory bowel disease and lupus were independently associated with osteonecrosis, but there was a similar dose relationship between glucocorticoids and osteonecrosis among adults with low-risk and high-risk diseases.
CONCLUSIONS
Glucocorticoid use was clearly associated with osteonecrosis in a dose-related fashion in adults, especially young adults, but this risk was not detectable in children. The absolute risk of glucocorticoid-associated osteonecrosis in the general paediatric population and in adults taking low glucocorticoid doses is at most extremely small.
目的
我们研究了患有各种慢性炎症性疾病的个体使用口服糖皮质激素与骨坏死(一种罕见但严重的骨病)之间的关系。我们假设在成年人与儿童以及自身免疫性疾病患者中会发现更强的关联。
设计
回顾性队列研究。
背景
来自英国全科医疗的具有人群代表性的数据(1994 - 2013年)。
参与者
被诊断患有哮喘、炎症性肠病、青少年、银屑病或类风湿性关节炎、银屑病或系统性红斑狼疮的儿童和成年人。
暴露因素
口服糖皮质激素模式。
主要和次要结局指标
确诊的骨坏死(主要)以及骨坏死加上临床特征(如症状、止痛药物、手术修复)(次要)。离散时间失效模型估计了口服糖皮质激素暴露后发生骨坏死的调整风险比(aHR)。由于糖皮质激素不太可能具有保护作用,假设检验为单侧检验(对应90%置信区间)。
结果
在对人口统计学、疾病相关和健康利用因素进行调整后,糖皮质激素暴露与成年人骨坏死相关(18 - 49岁,aHR 2.1(90%置信区间1.5至2.9);≥50岁,aHR 1.3(90%置信区间1.01至1.7))。然而,低剂量糖皮质激素,即平均剂量<7.5毫克泼尼松龙/天且最大剂量<30毫克/天,与成年人骨坏死无关。此外,即使在高糖皮质激素剂量下,也没有证据表明糖皮质激素暴露儿童的骨坏死增加(年龄交互作用p = 0.04)(任何糖皮质激素暴露,2 - 9岁:aHR 1.1(90%置信区间0.7至1.7);10 - 17岁:aHR 0.6(90%置信区间0.3至1.6))。关节炎、炎症性肠病和狼疮与骨坏死独立相关,但在低风险和高风险疾病的成年人中,糖皮质激素与骨坏死之间存在相似的剂量关系。
结论
糖皮质激素的使用在成年人,尤其是年轻成年人中显然与骨坏死呈剂量相关,但在儿童中未发现这种风险。在一般儿科人群和服用低剂量糖皮质激素的成年人中,糖皮质激素相关骨坏死的绝对风险至多极小。
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