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The Clinical Use of Denosumab for the Management of Low Bone Mineral Density In Postmenopausal Women

机译:地诺单抗治疗绝经后女性低骨矿物质密度的临床应用

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摘要

Osteoporosis is a leading cause of debility and declining quality of life in postmenopausal women worldwide. Treatment of osteoporosis has been ubiquitous throughout the developed world since the mid-1990s, most notably with the introduction of bisphosphonates in 1995. Nonetheless, the incidence of hip fractures increased by 25% between 1990 and 2000, despite advances in osteoporosis therapy. Studies indicate that bone density increases over the first 3 years of bisphosphonate therapy and then plateaus or perhaps even declines, placing these patients at greater risk of fracture. Since hip fractures are associated with increased morbidity, mortality, and increased cost of health care, improvements in treating osteoporosis are critical. Denosumab is a novel monoclonal antibody targeted against the receptor activator of nuclear factor-KB ligand (RANKL) that inhibits osteo-clast activity. Initial data suggest that denosumab increases bone mineral density for greater than 3 years. Of greater importance, denosumab has been shown to decrease vertebral fractures by 68%, nonvertebral fractures by 19%, and hip fractures by 42% for at least 36 months. Data also indicate that the safety profile of denosumab is equivalent to other drugs used in osteoporosis management, but potential risks of immunosuppression and cancer have been hypothesized.
机译:骨质疏松症是全世界绝经后妇女残疾和生活质量下降的主要原因。自从1990年代中期以来,骨质疏松症的治疗在整个发达国家已经无处不在,最显着的是在1995年引入了双膦酸盐。尽管如此,尽管骨质疏松症的治疗取得了进步,但髋部骨折的发生率在1990年至2000年之间增加了25%。研究表明,在双膦酸盐治疗的前3年中,骨密度增加,然后达到平稳甚至下降,使这些患者发生骨折的风险更高。由于髋部骨折与发病率,死亡率增加和医疗保健费用增加有关,因此改善骨质疏松症的治疗至关重要。 Denosumab是针对核因子-KB配体(RANKL)的受体活化剂的新型单克隆抗体,该受体可抑制破骨细胞的活性。初步数据表明,地诺单抗可增加骨矿物质密度3年以上。更重要的是,狄诺塞麦已显示在至少36个月内减少了68%的椎骨骨折,19%的非椎骨骨折和42%的髋部骨折。数据还表明,地诺单抗的安全性与骨质疏松症治疗中使用的其他药物相同,但已经假设存在免疫抑制和癌症的潜在风险。

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