Prompt clinical and biochemical response to denosumab in a young adult patient with craniofacial fibrous dysplasia.

Q3 Medicine Clinical Cases in Mineral and Bone Metabolism Pub Date : 2016-09-01 Epub Date: 2017-02-10 DOI:10.11138/ccmbm/2016.13.3.253
Cristina Eller-Vainicher, Diego Sergio Rossi, Giuseppe Guglielmi, Giada Anna Beltramini, Elisa Cairoli, Antonio Russillo, Giovanna Mantovani, Anna Spada, Iacopo Chiodini
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引用次数: 27

Abstract

Background: We report on the clinical and biochemical outcomes in a 20-year-old male suffering from active craniofacial monostotic fibrous dysplasia (MFD) of the left mandible treated with the RANK-L inhibitor, denosumab, following unsatisfactory responses to prior long-term bisphosphonates therapy.

Results: The patient had been treated over 9 years with pamidronate (cumulative dose of 810 mg) with incomplete control of pain. Following initiation of denosumab 60 mg subcutaneously, bone pain and bone turnover markers (osteocalcin, total and bone alkaline phosphatase and carboxy-terminal cross-linking telopeptide of type I collagen) were monitored over a 27 months period. Few hours after the first administration, the patient demonstrated a complete pain disappearance and after 4 weeks bone turnover markers fell within the normal range. Three months after denosumab initiation the patient reported a pain reactivation that required a second administration, which again led to the pain disappearance. Subsequently, denosumab was administered according to the pain reappearance and the injection was always followed by complete pain relief. However, a gradual shortening of the pain-free interval between administrations was observed, ranging from 90 to 75 days. All bone turnover markers stayed in the lower half of the normal range, even at the moment of pain reappearance, suggesting that the effect of denosumab on pain depends on mechanisms other than bone resorption suppression. No side effects were reported by the patient during the follow-up.

Conclusion: Denosumab appears to be effective in reducing bone turnover and bone pain in adult patients with active MFD.

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一名颅面纤维发育不良的年轻成人患者对地诺单抗的临床和生化反应迅速。
背景:我们报告了一名20岁男性左下颌骨活动性颅面单性纤维发育不良(MFD)患者的临床和生化结果,该患者接受RANK-L抑制剂denosumab治疗,此前长期双膦酸盐治疗效果不理想。结果:患者接受帕米膦酸钠治疗9年,累计剂量810 mg,疼痛不完全控制。在denosumab 60mg皮下注射后,在27个月的时间里监测骨痛和骨转换标志物(骨钙素、总碱性磷酸酶和骨碱性磷酸酶以及I型胶原的羧基末端交联端肽)。第一次给药后数小时,患者疼痛完全消失,4周后骨转换指标降至正常范围内。在denosumab启动3个月后,患者报告疼痛再激活,需要第二次给药,这再次导致疼痛消失。随后,根据疼痛重现情况给予地诺单抗,并始终在注射后完全缓解疼痛。然而,观察到两次给药之间的无痛间隔逐渐缩短,从90天到75天不等。所有骨转换指标都保持在正常范围的下半部分,即使在疼痛重现的那一刻,这表明denosumab对疼痛的影响取决于骨吸收抑制以外的机制。在随访期间,患者未报告任何副作用。结论:Denosumab可有效减少成年活动性MFD患者的骨转换和骨痛。
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Clinical Cases in Mineral and Bone Metabolism
Clinical Cases in Mineral and Bone Metabolism ENDOCRINOLOGY & METABOLISM-
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期刊介绍: The Journal encourages the submission of case reports and clinical vignettes that provide new and exciting insights into the pathophysiology and characteristics of disorders related to skeletal function and mineral metabolism and/or highlight pratical diagnostic and /or therapeutic considerations.
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