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使用罗莫索单抗和双膦酸盐治疗后出现的非典型股骨骨折。

Atypical femur fracture following romosozumab and bisphosphonate treatment.

作者信息

Jacunski Mark, Johnsson Hanna, Ralston Stuart H, Hauser Barbara

机构信息

Rheumatic Diseases Unit, NHS Lothian, Western General Hospital, Edinburgh, UK.

Centre for Genomic and Experimental Medicine, MRC Institute of Genetics and Cancer, Western General Hospital, Edinburgh, UK.

出版信息

J R Coll Physicians Edinb. 2025 Mar;55(1):19-22. doi: 10.1177/14782715241301487. Epub 2024 Nov 23.

Abstract

Romosozumab, a monoclonal antibody against sclerostin, is a newly licensed dual-acting osteoporosis treatment for patients at very high risk of fracture. Sclerostin inhibition leads to stimulation of bone formation and simultaneous inhibition of bone resorption. Only three cases of atypical femur fractures were reported out of 5,621 patients who received romosozumab in the pivotal randomised controlled trials FRAME and ARCH; however, most enrolled clinical trial patients were osteoporosis treatment-naïve or had a prolonged washout period. We report a case of an atypical femur fracture that occurred after the completion of romosozumab treatment which was followed by one dose of 5 mg intravenous zoledronic acid. The patient had previously received a 2-year course of subcutaneous teriparatide and subsequent three consecutive yearly intravenous zoledronic acid infusions, followed by a 2-year treatment break. This case highlights the risks of prolonged suppression of bone resorption, which includes romosozumab due to its dual action and the need for further research on how to minimise such deleterious medication effects. Patients who are switched from prolonged antiresorptive treatment to romosozumab, should be risk-assessed and counselled for the risk of atypical femur fracture.

摘要

罗莫单抗是一种抗硬化蛋白单克隆抗体,是一种新获批用于骨折高风险患者的双效骨质疏松症治疗药物。抑制硬化蛋白可刺激骨形成并同时抑制骨吸收。在关键随机对照试验FRAME和ARCH中,接受罗莫单抗治疗的5621例患者中仅报告了3例非典型股骨骨折;然而,大多数纳入临床试验的患者既往未接受过骨质疏松症治疗或有较长的洗脱期。我们报告1例患者在完成罗莫单抗治疗后发生非典型股骨骨折,随后接受了1剂5mg静脉注射唑来膦酸。该患者此前接受了2年皮下注射特立帕肽治疗,随后连续3年每年静脉输注唑来膦酸,之后有2年的治疗中断期。该病例突出了长期抑制骨吸收的风险,其中包括罗莫单抗因其双重作用所致的风险,以及需要进一步研究如何将此类有害药物效应降至最低。从长期抗吸收治疗转换为罗莫单抗治疗的患者,应进行风险评估并就非典型股骨骨折风险提供咨询。

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