Anti-sclerostin antibodies: a new frontier in fragility fractures treatment.

IF 3.4 2区 医学 Q2 RHEUMATOLOGY Therapeutic Advances in Musculoskeletal Disease Pub Date : 2023-01-01 DOI:10.1177/1759720X231197094
Giovanni Iolascon, Sara Liguori, Marco Paoletta, Giuseppe Toro, Antimo Moretti
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引用次数: 1

Abstract

Bone fragility is the determinant of the increased risk of minimal trauma fracture and must be treated with a multimodal approach that includes pharmacological therapy, physical exercise, and adequate nutrition. Pharmacological therapy, to date based on the administration of antiresorptive drugs, such as bisphosphonates and denosumab, or osteoanabolic drugs, such as teriparatide and abaloparatide, has shown to be effective in reducing the risk of fracture in osteoporotic patients. In the context of the cellular and molecular mechanisms that regulate bone metabolism, the discovery of the Wnt signaling pathway and its role in bone tissue homeostasis has allowed the identification of sclerostin as an inhibitor of osteoblastic activity and simultaneously as a stimulator of osteoclastic activity. Therefore, the use of a monoclonal antibody, romosozumab, against this protein has been tested as a potential drug with a dual action, stimulating bone neo-apposition and inhibiting bone resorption. The efficacy of romosozumab has been demonstrated in numerous clinical trials against both placebo and other drugs commonly used in the treatment of patients affected by osteoporosis. The advantages of this drug lie above all in its rapid action which makes it particularly suitable in clinical situations where it is necessary to improve bone strength very quickly due to the imminent risk of fragility fracture. Clinical studies and guidelines suggest romosozumab as an initial drug in an ideal sequential approach from osteoanabolic to antiresorptive drugs. Some aspects of cardiovascular safety remain to be fully investigated, therefore its use in osteoporotic patients at high cardiovascular risk should be avoided until further data become available.

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抗硬化蛋白抗体:脆性骨折治疗的新前沿。
骨脆性是导致最小创伤性骨折风险增加的决定因素,必须采用包括药物治疗、体育锻炼和充足营养在内的多模式治疗方法。迄今为止,基于抗吸收药物(如双膦酸盐和denosumab)或骨合成代谢药物(如teriparatide和abaloparatide)的药物治疗已被证明可有效降低骨质疏松症患者骨折的风险。在调节骨代谢的细胞和分子机制的背景下,Wnt信号通路及其在骨组织稳态中的作用的发现使我们能够确定硬化蛋白是成骨细胞活性的抑制剂,同时也是破骨细胞活性的刺激剂。因此,针对该蛋白的单克隆抗体romosozumab已被测试为具有双重作用的潜在药物,刺激骨新沉积和抑制骨吸收。在许多临床试验中,romosozumab的疗效已被证明可以对抗安慰剂和其他骨质疏松症患者常用的治疗药物。这种药物的优点首先在于它的快速作用,这使得它特别适合于临床情况下,需要非常迅速地提高骨强度,因为即将发生脆性骨折的风险。临床研究和指南建议将romosozumab作为从骨合成代谢药物到抗骨吸收药物的理想顺序方法的初始药物。心血管安全性的某些方面仍有待充分研究,因此在获得进一步的数据之前,应避免将其用于心血管风险高的骨质疏松症患者。
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来源期刊
CiteScore
6.80
自引率
4.80%
发文量
132
审稿时长
18 weeks
期刊介绍: Therapeutic Advances in Musculoskeletal Disease delivers the highest quality peer-reviewed articles, reviews, and scholarly comment on pioneering efforts and innovative studies across all areas of musculoskeletal disease.
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