Glucocorticoid exposure and fracture risk in patients with new-onset rheumatoid arthritis

被引:74
作者
Balasubramanian, A. [1 ]
Wade, S. W. [2 ]
Adler, R. A. [3 ,4 ]
Lin, C. J. F. [1 ]
Maricic, M. [5 ]
O'Malley, C. D. [1 ]
Saag, K. [6 ]
Curtis, J. R. [6 ]
机构
[1] Amgen Inc, Thousand Oaks, CA 91320 USA
[2] Wade Outcomes Res & Consulting, 358 South 700 East,Suite B 432, Salt Lake City, UT USA
[3] McGuire Vet Affairs Med Ctr, Richmond, VA USA
[4] Virginia Commonwealth Univ, Richmond, VA USA
[5] Univ Arizona, Sch Med, Tucson, AZ USA
[6] Univ Alabama Birmingham, Div Clin Immunol & Rheumatol, Birmingham, AL 35294 USA
关键词
Fracture; Glucocorticoids; Health services research; Osteoporosis; Rheumatoid arthritis; BONE-MINERAL DENSITY; INDUCED-OSTEOPOROSIS; ORAL CORTICOSTEROIDS; VERTEBRAL FRACTURES; CLAIMS DATA; DISEASE; THERAPY; COHORT; RECOMMENDATIONS; IDENTIFICATION;
D O I
10.1007/s00198-016-3646-z
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Retrospective claims analysis indicated that high levels of daily and cumulative doses of systemic glucocorticoids were associated with elevated fracture risk in a large cohort of new RA patients under age 65. Heightened risk began to decline within months of discontinuation. Findings were similar among patients age <50 years. Introduction We evaluated the impact of systemic glucocorticoid exposure on fracture risk among relatively young patients with new-onset rheumatoid arthritis (RA). Methods Using administrative data, we identified 42,127 RA patients diagnosed January 1, 2005-December 31, 2012, age 18-64 years, with benefits coverage for >= 12 months before RA diagnosis. Follow-up extended to clinical fracture, cancer diagnosis, or December 31, 2012. Glucocorticoid users were new to therapy. Fracture incidence rates (IR) were stratified by glucocorticoid exposure expressed as prednisone equivalent doses. Cox's proportional hazards models estimated fracture risk adjusted for demographics and baseline clinical characteristics to assess dose-response relationships with current (daily) and prior (cumulative) dose, and by time since discontinuation. Results Most patients (85 %) had glucocorticoid exposure. Exposed and unexposed patients were demographically similar (74 % female; mean age 49.7 and 48.8 years); 1 % had prior fracture. Fracture IRs (95% confidence intervals) were 5 to 9 per 1000 person-years at doses < 15 mg/day, 16.0 (11.0, 22.6) at doses >= 15 mg/day, and 13.4 (10.7, 16.7) at cumulative doses >= 5400 mg. Adjusted fracture risk was approximately 2-fold higher at highest dose levels compared with 0 mg/day current daily dose and < 675 mg cumulative dose, respectively. Fracture risk was 29 % lower at 60-182 days post-discontinuation compared with ongoing use and was similar to unexposed patients by 12 months. Findings were similar among patients age < 50 years. Conclusions Among younger, new-onset RA patients, fracture risk was significantly elevated at high levels of daily and cumulative dose, and was similar to unexposed patients by 12 months post-discontinuation.
引用
收藏
页码:3239 / 3249
页数:11
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