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在糖皮质激素治疗的最初 90 天内,平均每日糖皮质激素剂量、处方天数和累积剂量与随后的髋部和临床椎体骨折风险相关:一项使用日本全国医疗保险索赔数据库的回顾性队列研究。

Average daily glucocorticoid dose, number of prescription days, and cumulative dose in the initial 90 days of glucocorticoid therapy are associated with subsequent hip and clinical vertebral fracture risk: a retrospective cohort study using a nationwide health insurance claims database in Japan.

机构信息

Department of Public Health, Kindai University Faculty of Medicine, 377-2 Oono-Higashi, Osaka-Sayama, Osaka, 589-8511, Japan.

National Database Japan-Osteoporosis Management (NDBJ-OS) Study Group, Department of Public Health, Kindai University Faculty of Medicine, 377-2 Oono-Higashi, Osaka-Sayama, Osaka, 589-8511, Japan.

出版信息

Osteoporos Int. 2024 May;35(5):805-818. doi: 10.1007/s00198-024-07023-6. Epub 2024 Jan 24.

Abstract

PURPOSE

Fracture risk assessment is recommended at three months after glucocorticoid (GC) therapy initiation. This study aimed to assess whether GC exposure in the initial 90 days of GC therapy is associated with subsequent hip and clinical vertebral fracture risk using the nationwide health insurance claims database of Japan (NDBJ).

METHODS

Patients aged 50 years who were prescribed GC (≥ 70 mg prednisolone or equivalent; PSL) in the initial 90 days of GC therapy and were followed for hip and clinical vertebral fracture incidences for the subsequent 1080 days were selected from NDBJ. Associations of GC exposure with hip or clinical vertebral fracture risk were evaluated by Cox regression analysis adjusted for potential confounders.

RESULTS

We selected 316,396 women and 299,871 men for the GC-exposed group and 43,164 women and 33,702 men for the reference group. Higher GC doses and longer prescription days in the initial 90 days of GC therapy were significantly and dose-dependently associated with increased fracture risk relative to the reference group. Patients receiving GC 5 mg PSL/day had a significantly increased fracture risk in the stratum of 30-59 days of GC prescription. In addition, female patients who received GC (≥ 1 and < 2.5 mg PSL/day) for 90 days in the initial 90 days of GC therapy had a significantly increased fracture risk.

CONCLUSIONS

GC exposure in the initial 90 days of GC therapy was dose-dependently associated with hip and clinical vertebral fracture risk. GC may increase fracture risk with lower doses for shorter durations than previously reported. Fracture risk assessment three months after glucocorticoid (GC) therapy initiation is recommended. We found that GC exposure in the initial 90 days of GC therapy at lower daily doses for shorter durations than previously reported were significantly and dose-dependently associated with fracture risk using a nationwide health insurance claims database.

摘要

目的

建议在糖皮质激素(GC)治疗开始后三个月进行骨折风险评估。本研究旨在使用日本全国医疗保险索赔数据库(NDBJ)评估 GC 治疗初始 90 天内的 GC 暴露与随后髋部和临床椎体骨折风险之间的关系。

方法

从 NDBJ 中选择在 GC 治疗初始 90 天内接受 GC(泼尼松龙≥70mg 或等效药物;PSL)治疗且在随后的 1080 天内随访髋部和临床椎体骨折发生率的年龄≥50 岁的患者。通过 Cox 回归分析调整潜在混杂因素评估 GC 暴露与髋部或临床椎体骨折风险的相关性。

结果

我们选择了 316396 名女性和 299871 名男性纳入 GC 暴露组,43164 名女性和 33702 名男性纳入对照组。GC 治疗初始 90 天内的 GC 剂量较高和处方天数较长与骨折风险显著相关,且呈剂量依赖性。接受 5mg PSL/天 GC 治疗的患者在 GC 处方 30-59 天的亚组中骨折风险显著增加。此外,GC 治疗初始 90 天内接受 GC(≥1 至<2.5mg PSL/天)治疗 90 天的女性患者骨折风险显著增加。

结论

GC 治疗初始 90 天内的 GC 暴露与髋部和临床椎体骨折风险呈剂量依赖性相关。GC 可能会增加骨折风险,所需的剂量和持续时间比之前报道的要短。建议在糖皮质激素(GC)治疗开始后三个月进行骨折风险评估。我们发现,与之前报道的相比,在 GC 治疗的初始 90 天内,较低的日剂量和较短的治疗时间内,GC 暴露与骨折风险呈显著且剂量依赖性相关,这是使用全国健康保险索赔数据库得出的结果。

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