Efficacy and safety of candidate biosimilar CT-P41 versus reference denosumab: a double-blind, randomized, active-controlled, Phase 3 trial in postmenopausal women with osteoporosis.

IF 4.2 2区医学 Q1 ENDOCRINOLOGY & METABOLISM

Osteoporosis International Pub Date : 2024-11-01 Epub Date: 2024-07-23 DOI:10.1007/s00198-024-07161-x

Jean-Yves Reginster, Edward Czerwinski, Krzysztof Wilk, Przemysław Borowy, Anna Strzelecka, Tomasz Budlewski, Monika Janowska-Maus, Krzysztof Szymanowski, Joanna Kwiatek, Svitlana Postol, Airi Põder, Jerzy Supronik, SungHyun Kim, JeeHye Suh, NooRi Han, NaHyun Kim, SeoHee Bae, Stuart L Silverman

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Abstract

This 78-week (18-month) study conducted in 479 postmenopausal women with osteoporosis evaluated the efficacy, pharmacodynamics, pharmacokinetics, safety, and immunogenicity of candidate biosimilar CT-P41 relative to US reference denosumab. CT-P41 had equivalent efficacy and pharmacodynamics to US-denosumab, with similar pharmacokinetics and comparable safety and immunogenicity profiles.

Purpose: To demonstrate equivalence of candidate biosimilar CT-P41 and US reference denosumab (US-denosumab) in postmenopausal women with osteoporosis.

Methods: This 78-week (18-month), double-blind, randomized, active-controlled Phase 3 study (NCT04757376) comprised two treatment periods (TPs). In TPI, patients (N = 479) were randomized 1:1 to 60 mg subcutaneous CT-P41 or US-denosumab. At Week 52, those who had received CT-P41 in TPI continued to do so. Those who had received US-denosumab were randomized (1:1) to continue treatment or switch to CT-P41 in TPII. The primary efficacy endpoint was percent change from baseline in lumbar spine bone mineral density at Week 52. Efficacy equivalence was concluded if associated 95% confidence intervals (CI) for least squares (LS) mean group differences fell within ± 1.503%. The primary pharmacodynamic (PD) endpoint was area under the effect curve for serum carboxy-terminal cross-linking telopeptide of type I collagen through the first 26 weeks, with an equivalence margin of 80-125% (for 95% CIs associated with geometric LS mean ratios).

Results: Equivalence was demonstrated for CT-P41 and US-denosumab with respect to primary efficacy (LS mean difference [95% CI]: - 0.139 [- 0.826, 0.548] in the full analysis set and - 0.280 [- 0.973, 0.414] in the per-protocol set) and PD (geometric LS mean ratio [95% CI]: 94.94 [90.75, 99.32]) endpoints. Secondary efficacy, PD, pharmacokinetics, and safety results were comparable among all groups up to Week 78, including after transitioning to CT-P41 from US-denosumab.

Conclusions: CT-P41 was equivalent to US-denosumab in women with postmenopausal osteoporosis, with respect to primary efficacy and PD endpoints.

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候选生物仿制药 CT-P41 与参考药物地诺单抗的疗效和安全性：针对绝经后骨质疏松症妇女的双盲、随机、主动对照 3 期试验。

这项为期 78 周（18 个月）的研究在 479 名绝经后骨质疏松症妇女中进行，评估了候选生物仿制药 CT-P41 相对于美国参考药物地诺单抗的疗效、药效学、药代动力学、安全性和免疫原性。CT-P41与US-denosumab具有同等的疗效和药效动力学，药代动力学相似，安全性和免疫原性也相当。目的：证明在绝经后骨质疏松症女性患者中，候选生物类似药CT-P41与美国参考药denosumab（US-denosumab）具有同等疗效：这项为期78周（18个月）的双盲、随机、主动对照3期研究（NCT04757376）包括两个治疗期（TP）。在TPI中，患者（479人）按1:1的比例随机接受60毫克皮下CT-P41或US-denosumab治疗。第52周时，在TPI期间接受过CT-P41治疗的患者继续接受治疗。接受过 US-denosumab 治疗的患者按 1:1 随机分配继续接受治疗或在 TPII 中改用 CT-P41。主要疗效终点是第 52 周时腰椎骨矿物质密度与基线相比的百分比变化。如果相关的最小二乘法 (LS) 平均组间差异的 95% 置信区间 (CI) 在 ± 1.503% 以内，则得出疗效等效的结论。主要药效学 (PD) 终点是前 26 周血清 I 型胶原蛋白羧基末端交联端肽的效应曲线下面积，等效幅度为 80-125%（与几何 LS 均值比相关的 95% CI）：CT-P41和US-denosumab的主要疗效（LS均值差异[95% CI]：全分析组为- 0.139 [- 0.826, 0.548]，按方案分析组为- 0.280 [- 0.973, 0.414]）和PD（几何LS均值比[95% CI]：94.94 [90.75, 99.32]）终点均为等效。在第78周之前，包括从US-denosumab过渡到CT-P41之后，各组的次要疗效、PD、药代动力学和安全性结果相当：结论：对于绝经后骨质疏松症妇女，CT-P41与US-denosumab在主要疗效和PD终点方面具有同等疗效。

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来源期刊

Osteoporosis International 医学-内分泌学与代谢

CiteScore

8.10

自引率

10.00%

发文量

224

审稿时长

3 months

期刊介绍： An international multi-disciplinary journal which is a joint initiative between the International Osteoporosis Foundation and the National Osteoporosis Foundation of the USA, Osteoporosis International provides a forum for the communication and exchange of current ideas concerning the diagnosis, prevention, treatment and management of osteoporosis and other metabolic bone diseases. It publishes: original papers - reporting progress and results in all areas of osteoporosis and its related fields; review articles - reflecting the present state of knowledge in special areas of summarizing limited themes in which discussion has led to clearly defined conclusions; educational articles - giving information on the progress of a topic of particular interest; case reports - of uncommon or interesting presentations of the condition. While focusing on clinical research, the Journal will also accept submissions on more basic aspects of research, where they are considered by the editors to be relevant to the human disease spectrum.