地舒单抗治疗对骨质疏松症患者骨密度和骨转换标志物的影响:真实世界经验 2 年随访。
Effect of denosumab treatment on bone mineral density and bone turnover markers in osteoporotic patients: real-life experience 2-year follow-up.
机构信息
Department of Endocrinology and Metabolism, Marmara University School of Medicine, Istanbul, Turkey.
Department of Radiology, Marmara University School of Medicine, Istanbul, Turkey.
出版信息
Arch Osteoporos. 2022 Sep 17;17(1):125. doi: 10.1007/s11657-022-01145-2.
UNLABELLED
Denosumab leads to improvements in BMD levels and is a well-tolerated agent according to results of randomized controlled studies but results in real-life setting are important to evaluate drug adherence and real-life efficiency. In this study, we present the results of 305 patients that were treated with denosumab in our clinic.
INTRODUCTION
The long-term efficacy of anti-osteoclastic drugs in treatment of osteoporosis is well known. Denosumab, a novel human monoclonal antibody, is an anti-osteoclastic agent that has been shown to lead to reductions in vertebral, nonvertebral, and hip fracture risk in randomized and observational studies. Real-life data of this agent is increasing. In this study, we presented our real-life data about the 2-year follow-up of patients under denosumab treatment.
METHODS
Osteoporotic patients who were treated with at least one denosumab injection between 2014 and 2020 years were included. Clinical and demographic data, bone turnover markers, and radiological reports (bone mineral densitometry (BMD), vertebral x-ray) were obtained from patient files retrospectively.
RESULTS
A total of 305 patients (f/m: 275/30, 68.1 ± 11.05 years) were included. The median injection number was 4 (1-10). Two hundred seventy-three patients (89.8%) were persistent on treatment at the 12th month; 175 patients (57.3%) were persistent at 24th month. Sixty-eight patients (22%) were not using denosumab anymore, 55 of the patients were not continuing by doctor desicion and 13 were not continuing due to patient-related causes. Median BMD levels significantly increased from 0.809 (0.2-1.601, IQR: 0.136) to 0.861 (0.517-1.607, IQR: 0.14) in L1-L4 and from 0.702 (0.349-0.997, IQR: 0.125) to 0.745 (0.508-1.008, IQR: 0.137) in femur area at the 24th month of treatment. An improvement of 8.04% in L1-L4 BMD and 4.5% in femur neck BMD levels at the 24th month of treatment was observed. There was a significant decrease in bone turnover markers at the 24th month of treatment.
CONCLUSION
In our group of patients under denosumab treatment, 53% of persistence was found at 24 months and associated with improvement in BMD levels without any significant side effects except one case with urticarial reaction. Denosumab leads to improvements in BMD levels and is a well-tolerated agent in a real-life setting comparable to results of randomized controlled studies in patients with different comorbidities.
目的
根据随机对照研究的结果,地舒单抗可提高骨密度水平并具有良好的耐受性,但在真实环境中的结果对于评估药物依从性和真实疗效很重要。本研究报告了在我们诊所接受地舒单抗治疗的 305 例患者的结果。
方法
本研究纳入了 2014 年至 2020 年期间至少接受过一次地舒单抗注射的骨质疏松症患者。回顾性从患者病历中获取临床和人口统计学数据、骨转换标志物以及影像学报告(骨密度、椎体 X 射线)。
结果
共纳入 305 例患者(女性/男性:275/30,68.1±11.05 岁)。中位注射次数为 4 次(1-10 次)。273 例(89.8%)患者在第 12 个月时仍持续治疗;175 例(57.3%)患者在第 24 个月时仍持续治疗。68 例(22%)患者不再使用地舒单抗,55 例患者因医生决定而停止治疗,13 例患者因患者相关原因而停止治疗。治疗第 24 个月时,L1-L4 骨密度中位数从 0.809(0.2-1.601,IQR:0.136)增加到 0.861(0.517-1.607,IQR:0.14),股骨区域骨密度中位数从 0.702(0.349-0.997,IQR:0.125)增加到 0.745(0.508-1.008,IQR:0.137)。治疗第 24 个月时,L1-L4 骨密度增加 8.04%,股骨颈骨密度增加 4.5%。治疗第 24 个月时,骨转换标志物显著下降。
结论
在接受地舒单抗治疗的患者中,24 个月时的持续率为 53%,且与骨密度水平的改善相关,无明显不良反应,仅 1 例出现荨麻疹反应。地舒单抗可提高骨密度水平,在真实环境中具有良好的耐受性,与不同合并症患者的随机对照研究结果相当。
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