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骨髓瘤相关骨病的新兴治疗方法。

Emerging treatment approaches for myeloma-related bone disease.

机构信息

a Department of Clinical Therapeutics , National and Kapodistrian University of Athens School of Medicine , Athens , Greece.

出版信息

Expert Rev Hematol. 2017 Mar;10(3):217-228. doi: 10.1080/17474086.2017.1283213. Epub 2017 Jan 29.

DOI:10.1080/17474086.2017.1283213
PMID:28092987
Abstract

Multiple myeloma is characterized by the presence of osteolytic lesions that leads to devastating skeletal-related events in the majority of patients. Myeloma bone disease is attributed to increased osteoclastic and suppressed osteoblastic activity. Areas covered: Bisphosphonates remain the main treatment option, however they have limitations on their own. Understanding the pathogenesis of myeloma bone disease may provide a roadmap for new therapeutic approaches. The pathway of RANKRANKLOPG pathway has revealed denosumab, a monoclonal antibody targeting RANKL as a novel emerging therapy for myeloma-related bone disease. Furthermore, the Wnt signaling inhibitors dicckopf-1 and sclerostin that are implicated in the pathogenesis of bone destruction of myeloma are now targeted by novel monoclonal antibodies. Activin-A is a TGF-beta superfamily member which increases osteoclast activity and inhibits osteoblast function in myeloma; sotatercept and other molecules targeting activin-A have entered into clinical development. Several other molecules and pathways that play an important role in the pathogenesis of bone destruction in myeloma, such as periostin, adiponectin, Notch and BTK signaling are also targeted in an attempt to develop novel therapies for myeloma-related bone disease. Expert commentary: We summarize the current advances in the biology of myeloma bone disease and the potential therapeutic targets.

摘要

多发性骨髓瘤的特征是存在溶骨性病变,这导致大多数患者发生破坏性的骨骼相关事件。骨髓瘤骨病归因于破骨细胞活性增加和成骨细胞活性受抑制。涵盖的领域:双膦酸盐仍然是主要的治疗选择,但它们本身存在局限性。了解骨髓瘤骨病的发病机制可能为新的治疗方法提供路线图。RANK/RANKL/OPG 途径的发现,使针对 RANKL 的单克隆抗体地舒单抗成为一种新的骨髓瘤相关骨病治疗方法。此外,参与骨髓瘤骨破坏发病机制的 Dickkopf-1 和 Sclerostin 等 Wnt 信号抑制剂,现在也成为新型单克隆抗体的靶向治疗药物。激活素-A 是 TGF-β 超家族成员,可增加骨髓瘤中的破骨细胞活性并抑制成骨细胞功能;针对激活素-A 的 sotatercept 和其他分子已进入临床开发阶段。其他一些在骨髓瘤骨破坏发病机制中起重要作用的分子和途径,如骨膜蛋白、脂联素、Notch 和 BTK 信号通路,也被作为靶点,试图开发新的骨髓瘤相关骨病治疗方法。专家评论:我们总结了骨髓瘤骨病生物学和潜在治疗靶点的最新进展。

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