1型成骨不全症患者的骨质疏松症经romosozumab治疗得到改善

Antara Dattagupta MD, MEng , Steven Petak MD, JD
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引用次数: 1

摘要

背景/目的成骨不全症(osteogenesis imperfecta, OI)是一种影响1型胶原合成的遗传性疾病,可导致骨脆性增加、骨量降低和骨骼畸形。双膦酸盐被推荐用于OI患者的治疗;然而,硬化蛋白抑制剂如romosozumab在骨质疏松性成骨不全患者中的疗效尚未确定。病例报告:一名52岁的G2P2临床诊断为成骨不全,儿童期开始有多处骨折史,骨量低。体格检查可见蓝色巩膜。2014年4月至2015年6月,患者曾接受阿仑膦酸钠治疗,但骨密度(BMD)未见明显改善。绝经后,她开始罗莫索单抗210毫克皮下治疗,每月一次,持续12个月。重复双能x线骨密度测量显示脊柱骨密度增加10.3%,右髋关节骨密度增加5.4%。骨小梁评分提高5.2%。目前的文献对成骨不全症患者使用硬化蛋白抑制剂的研究有限。与治疗开始相比,我们的患者在接受romosozumab治疗后脊柱和右髋关节骨密度的改善达到95%的置信水平。她的骨小梁评分也明显改善。在我们的患者治疗6个月后,日本一例患有严重骨质疏松性成骨不全并复发性骨折的男性患者在接受romosozumab治疗后骨密度有所改善。结论:该病例突出了我们的患者对romosozumab的显著反应,值得进一步研究romosozumab作为OI合并骨质疏松患者的潜在治疗选择。
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Osteoporosis Improved by Romosozumab Therapy in a Patient With Type I Osteogenesis Imperfecta

Background/Objective

Osteogenesis imperfecta (OI) is a genetic disorder that affects type 1 collagen synthesis causing increased bone fragility, low bone mass, and skeletal deformity. Bisphosphonates are recommended for treatment of OI patients; however, the efficacy of sclerostin inhibitors such as romosozumab has not been determined in OI patients with osteoporosis.

Case Report

A 52-year-old G2P2 clinically diagnosed with OI, with a history of multiple fractures beginning in childhood presented with low bone mass. On physical examination, blue sclera was observed. She was previously treated with alendronate therapy from April 2014 to June 2015 without significant improvement in bone mineral density (BMD). After the onset of menopause, she began romosozumab 210 mg subcutaneous therapy once a month for 12 months. Repeat dual-energy X-ray absorptiometry showed an increase of 10.3% in BMD of the spine and a 5.4% increase in BMD of the right hip. The trabecular bone score increased by 5.2%.

Discussion

Current literature is limited regarding the use of sclerostin inhibitors in OI patients. Our patient’s improvement in BMD of the spine and right hip after romosozumab therapy was significant at a 95% confidence level, compared to treatment initiation. Her trabecular bone score also improved significantly. Six months into our patient’s treatment course, a case in Japan of a male with severe osteoporotic OI and recurrent fractures showed improvement in BMD after romosozumab therapy.

Conclusion

This case highlights our patient’s significant response to romosozumab and warrants further investigation of romosozumab as a potential treatment option for OI patients with osteoporosis.

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来源期刊
AACE Clinical Case Reports
AACE Clinical Case Reports Medicine-Endocrinology, Diabetes and Metabolism
CiteScore
2.30
自引率
0.00%
发文量
61
审稿时长
55 days
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