Severe Rebound-Associated Vertebral Fractures After Denosumab Discontinuation: 9 Clinical Cases Report

O. Lamy, Elena Gonzalez‐Rodriguez, D. Stoll, D. Hans, B. Aubry-Rozier
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引用次数: 153

Abstract

Context Denosumab inhibits bone resorption, increases bone mineral density, and reduces fracture risk. Denosumab was approved for the treatment of osteoporosis and the prevention of bone loss in some oncological situations. Denosumab discontinuation is associated with a severe bone turnover rebound (BTR) and a rapid loss of bone mineral density. The clinical consequences of the BTR observed after denosumab discontinuation are not known. Cases Description We report 9 women who presented 50 rebound-associated vertebral fractures (RAVFs) after denosumab discontinuation. A broad biological and radiological assessment excluded other causes than osteoporosis. These 9 cases are unusual and disturbing for several reasons. First, all vertebral fractures (VFs) were spontaneous, and most patients had a high number of VFs (mean = 5.5) in a short period of time. Second, the fracture risk was low for most of these women. Third, their VFs occurred rapidly after last denosumab injection (9-16 months). Fourth, vertebroplasty was associated with a high number of new VFs. All the observed VFs seem to be related to denosumab discontinuation and unlikely to the underlying osteoporosis or osteopenia. We hypothesize that the severe BTR is involved in microdamage accumulation in trabecular bone and thus promotes VFs. Conclusion Studies are urgently needed to determine 1) the pathophysiological processes involved, 2) the clinical profile of patients at risk for RAVFs, and 3) the management and/or treatment regimens after denosumab discontinuation. Health authorities, physicians, and patients must be aware of this RAVF risk. Denosumab injections must be scrupulously done every 6 months but not indefinitely.
地诺单抗停药后严重反弹相关椎体骨折9例临床报告
denosumab抑制骨吸收,增加骨矿物质密度,降低骨折风险。Denosumab被批准用于治疗骨质疏松症和预防某些肿瘤情况下的骨质流失。Denosumab停药与严重的骨转换反弹(BTR)和骨矿物质密度的快速损失有关。denosumab停药后观察到的BTR的临床后果尚不清楚。病例描述我们报告了9名妇女在denosumab停药后出现50例反弹相关椎体骨折(RAVFs)。广泛的生物学和放射学评估排除了骨质疏松症以外的其他原因。这9个案例不同寻常,令人不安的原因有几个。首先,所有椎体骨折(VFs)均为自发性骨折,且大多数患者在短时间内发生较多VFs(平均5.5)。其次,大多数女性的骨折风险较低。第三,在最后一次denosumab注射后(9-16个月),VFs发生迅速。第四,椎体成形术与大量新的VFs相关。所有观察到的VFs似乎都与denosumab停药有关,而不太可能与潜在的骨质疏松或骨质减少有关。我们假设严重的BTR参与了骨小梁的微损伤积累,从而促进了VFs。结论迫切需要研究1)所涉及的病理生理过程,2)ravf风险患者的临床概况,以及3)地诺单抗停药后的管理和/或治疗方案。卫生当局、医生和患者必须意识到这种RAVF风险。Denosumab注射必须每6个月进行一次,但不是无限期的。
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