Lee Chia-Che, Wang Chen-Yu, Hung Chih-Chien, Huang Chuan-Ching, Li Chung-Yi, Chen Hsuan-Yu, Chang Yun-Liang, Tseng Wo-Jan, Wang Ting-Ming, Yang Rong-Sen, Wong Tze-Hong, Fu Shau-Huai
Department of Orthopedic Surgery, National Taiwan University Hospital, Taipei, Taiwan.
School of Pharmacy, College of Medicine, National Taiwan University, Taipei, Taiwan.
Front Med (Lausanne). 2021 Sep 8;8:717168. doi: 10.3389/fmed.2021.717168. eCollection 2021.
Though denosumab is an effective treatment for osteoporosis, the rebound effect after discontinuation has drawn investigators' attention. It includes a dramatic loss of gained bone mineral density (BMD) and an increased risk of vertebral fractures. This prospective multi-institutional randomized controlled trial aims to investigate whether zoledronate prevents loss of BMD after discontinuation of denosumab. The trial was registered as Denosumab Sequential Therapy (DST) trial in March 2019 at clinicaltrials.gov, with the identifier NCT03868033. The study is conducted at National Taiwan University Hospital and its branches. Patients who have continuously received denosumab treatment for two or more years are surveyed for eligibility. Baseline characteristics and questionnaires of life quality are recorded after recruitment. BMD, circulating levels of bone turnover markers (BTMs), including serum N-terminal propeptide of type 1 collagen (P1NP) and C-terminal telopeptide (CTX), are checked before the stratified randomization to 4 groups. Biological sex and the T-scores are used to create 4 strata. The participants in group 1 adhere to regular denosumab therapy for another 2 years. All the other patients receive on-time zoledronate treatment in the first year. The participants in group 2, 3, and 4 have on-time denosumab, on-time zoledronate and drug holiday in the second year, respectively. BMDs are checked annually. Pre-scheduled checkpoints of BTMs are also arranged. For patient safety, rescue treatment with another injection of zoledronate will be applied to the patients on drug holiday if the CTX levels raise above the pre-specified threshold, 0.573 ng/mL for women and 0.584 ng/mL for men. The primary outcomes are the percentage changes of BMDs in lumbar spine, total hip and femoral neck. The secondary outcomes include the changes of serum level of the BTMs, new osteoporotic fractures, extra zoledronate injections needed in group 4 and the differences of quality of life. We aim to provide evidence whether zoledronate prevents bone loss after denosumab cessation. To our knowledge, the study has the largest sample size. No other randomized controlled study included all the three different treatment strategies and a positive control. It is also the first associated randomized controlled trial outside Europe.
尽管地诺单抗是治疗骨质疏松症的有效药物,但停药后的反弹效应已引起研究人员的关注。这包括已获得的骨矿物质密度(BMD)急剧下降以及椎体骨折风险增加。这项前瞻性多机构随机对照试验旨在研究唑来膦酸是否能预防地诺单抗停药后骨密度的流失。该试验于2019年3月在clinicaltrials.gov上注册为地诺单抗序贯治疗(DST)试验,标识符为NCT03868033。该研究在台湾大学医院及其分院进行。对连续接受地诺单抗治疗两年或更长时间的患者进行资格审查。招募后记录基线特征和生活质量问卷。在分层随机分为4组之前,检查骨密度、骨转换标志物(BTM)的循环水平,包括血清1型胶原N端前肽(P1NP)和C端肽(CTX)。根据生物性别和T值创建4个分层。第1组的参与者继续接受常规地诺单抗治疗2年。所有其他患者在第一年接受按时唑来膦酸治疗。第2组、第3组和第4组的参与者在第二年分别接受按时地诺单抗、按时唑来膦酸和停药治疗。每年检查骨密度。还安排了预先设定的骨转换标志物检查点。为了患者安全,如果CTX水平升高超过预先设定的阈值(女性为0.573 ng/mL,男性为0.584 ng/mL),将对停药患者再次注射唑来膦酸进行抢救治疗。主要结局是腰椎、全髋和股骨颈骨密度的百分比变化。次要结局包括骨转换标志物血清水平的变化、新发骨质疏松性骨折、第4组所需额外注射唑来膦酸的次数以及生活质量的差异。我们旨在提供证据证明唑来膦酸是否能预防地诺单抗停药后的骨质流失。据我们所知,该研究样本量最大。没有其他随机对照研究包括所有三种不同的治疗策略和一个阳性对照。这也是欧洲以外的首个相关随机对照试验。
