伊沙妥昔单抗加卡非佐米-地塞米松与卡非佐米-地塞米松治疗复发性多发性骨髓瘤患者(IKEMA):3期随机对照试验的总生存期分析。

IF 15.4 1区 医学 Q1 HEMATOLOGY
Lancet Haematology Pub Date : 2024-10-01 Epub Date: 2024-07-24 DOI:10.1016/S2352-3026(24)00148-0
Kwee Yong, Thomas Martin, Meletios-Athanasios Dimopoulos, Joseph Mikhael, Marcelo Capra, Thierry Facon, Roman Hajek, Ivan Špička, Ross Baker, Kihyun Kim, Gracia Martinez, Chang-Ki Min, Ludek Pour, Xavier Leleu, Albert Oriol, Youngil Koh, Kenshi Suzuki, France Casca, Sandrine Macé, Marie-Laure Risse, Philippe Moreau
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引用次数: 0

摘要

背景介绍伊沙妥昔单抗是一种抗 CD38 单克隆抗体,已被批准用于治疗复发或难治性多发性骨髓瘤。此前的IKEMA试验分析显示,与单独接受卡非佐米-地塞米松治疗的患者相比,接受伊沙妥昔单抗与卡非佐米-地塞米松联合治疗的多发性骨髓瘤患者的无进展生存期更长。在此,我们报告了IKEMA试验的总生存率分析:这项前瞻性、随机、开放标签、主动对照的三期研究纳入了来自北美、南美、欧洲和亚太地区 16 个国家 69 个研究中心的 18 岁或以上复发或难治性多发性骨髓瘤患者,这些患者之前接受过一至三期治疗。患者被随机分配(3:2)接受伊沙妥昔单抗加卡非佐米-地塞米松(伊沙妥昔单抗组)或卡非佐米-地塞米松(对照组)治疗。在伊沙妥昔单抗组,患者在第一个28天周期的第1、8、15和22天,以及随后的28天周期的第1和15天接受静脉注射伊沙妥昔单抗(10毫克/千克)。两个治疗组均静脉注射卡非佐米(20 毫克/平方米,第一个周期的第 1 天和第 2 天;56 毫克/平方米,第一个周期的第 8 天、第 9 天、第 15 天和第 16 天,以及随后周期的第 1 天、第 2 天、第 8 天、第 9 天、第 15 天和第 16 天)和静脉注射或口服地塞米松(20 毫克,第 1 天、第 2 天、第 8 天、第 9 天、第 15 天、第 16 天、第 22 天和第 23 天)。该试验的主要终点是无进展生存期,此前已有报道。治疗一直持续到病情进展、出现不可接受的毒性或患者要求停药为止。本文报告的总生存期分析计划在意向治疗人群的主要无进展生存期分析3年后进行。此外,还对下一次治疗时间和第二次无进展生存期等次要终点进行了分析。由于采用分层检验,报告的 p 值为非推断值。该试验已在ClinicalTrials.gov(NCT03275285)上注册:2017年11月15日至2019年3月21日期间,302名患者入组并随机分配:伊沙妥昔单抗组179人(59%),对照组123人(41%)。169名(56%)患者为男性,133名(44%)为女性,214名(71%)为白人,50名(17%)为亚裔,9名(3%)为黑人或非裔美国人,3名(1%)为多种族。在本次总生存期分析的数据截止日(2023年2月7日),伊沙妥昔单抗组发生了79例(44%)总生存期事件,对照组发生了59例(48%)总生存期事件(中位随访时间为56-61个月[IQR 54-90-58-02])。伊沙妥昔单抗组未达到中位总生存期(以月为单位)(NR;95% CI 52-17-NR),对照组为 50-60 个月(38-93-NR)(危险比 [HR] 0-855 [95% CI 0-608-1-202],名义单侧 p=0-18)。伊沙妥昔单抗组 48 个月的生存概率为 59-7%(95% CI 52-0-66-7),对照组为 52-2%(95% CI 42-7-60-8)(基于 Kaplan-Meier 分析)。观察到伊沙妥昔单抗组患者的下次治疗时间(HR 0-583 [95% CI 0-429-0-792],名义单侧 p=0-0002)和第二次无进展生存期(0-663 [0-491-0-895],名义单侧 p=0-0035)均有所改善。最常见的治疗突发不良事件是输液反应(伊沙妥昔单抗组82例[46%],对照组4例[3%])和上呼吸道感染(分别为71例[40%]和34例[28%])。尽管伊沙妥昔单抗组的患者多接受了30周的治疗,但两组患者因治疗引发的不良事件而终止治疗的情况相似(伊沙妥昔单抗组24例[14%],对照组22例[18%])。在研究治疗期间,伊沙妥昔单抗组有12名患者(7%)和对照组有6名患者(5%)发生了致命的治疗相关不良事件:目前的分析结果表明,治疗组之间的总生存率未发现差异,也未观察到新的安全信号。总体而言,证据表明伊沙妥昔单抗加卡非佐米-地塞米松是复发或难治性多发性骨髓瘤患者的主要治疗方法:资助方:赛诺菲公司
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Isatuximab plus carfilzomib-dexamethasone versus carfilzomib-dexamethasone in patients with relapsed multiple myeloma (IKEMA): overall survival analysis of a phase 3, randomised, controlled trial.

Background: Isatuximab is an anti-CD38 monoclonal antibody approved for the treatment of relapsed or refractory multiple myeloma. Previous analyses of the IKEMA trial showed prolonged progression-free survival in patients with this disease who received isatuximab in combination with carfilzomib-dexamethasone as compared with those who received carfilzomib-dexamethasone alone. Herein, we report the analysis of overall survival from the IKEMA trial.

Methods: This prospective, randomised, open-label, active-controlled, phase 3 study included patients with relapsed or refractory multiple myeloma aged 18 years or older, who had received one to three previous lines of treatment from 69 study centres in 16 countries across North America, South America, Europe, and the Asia-Pacific region. Patients were randomly allocated (3:2) to treatment with either isatuximab plus carfilzomib-dexamethasone (isatuximab group) or carfilzomib-dexamethasone (control group). In the isatuximab group, patients received intravenous isatuximab (10 mg/kg on days 1, 8, 15, and 22 of the first 28-day cycle, and days 1 and 15 of subsequent 28-day cycles). In both treatment groups, intravenous carfilzomib (20 mg/m2 on days 1 and 2 of the first cycle; and 56 mg/m2 on days 8, 9, 15, and 16 of the first cycle, and days 1, 2, 8, 9, 15, and 16 of subsequent cycles) and intravenous or oral dexamethasone (20 mg on days 1, 2, 8, 9, 15, 16, 22, and 23) were administered. The primary endpoint of the trial was progression-free survival, which was reported previously. Treatment continued until progression, unacceptable toxicity, or patient request to discontine. The overall survival analysis reported here was planned to be conducted 3 years after the primary progression-free survival analysis in the intention-to-treat population. Additional analyses were conducted on the secondary endpoints of time to next treatment and second-progression-free survival. Reported p values are non-inferential due to hierarchical testing. This trial is registered with ClinicalTrials.gov (NCT03275285).

Findings: Between Nov 15, 2017, and March 21, 2019, 302 patients were enrolled and randomly allocated: 179 (59%) to the isatuximab group and 123 (41%) to the control group. 169 (56%) patients were male, 133 (44%) were female, 214 (71%) were White, 50 (17%) were Asian, nine (3%) were Black or African American, and three (1%) were multiracial. At data cutoff for this overall survival analysis (Feb 7, 2023), 79 (44%) overall survival events in the isatuximab group and 59 (48%) in the control group had occurred (median follow-up 56·61 months [IQR 54·90-58·02]). Median overall survival (in months) was not reached (NR; 95% CI 52·17-NR) in the isatuximab group and was 50·60 months (38·93-NR) in the control group (hazard ratio [HR] 0·855 [95% CI 0·608-1·202], nominal one-sided p=0·18). Survival probability at 48 months was 59·7% (95% CI 52·0-66·7) in the isatuximab group and 52·2% (95% CI 42·7-60·8) in the control group (based on Kaplan-Meier analysis). Improvements in time to next treatment (HR 0·583 [95% CI 0·429-0·792], nominal one-sided p=0·0002) and second-progression-free survival (0·663 [0·491-0·895], nominal one-sided p=0·0035) were observed in the isatuximab group. The most common treatment-emergent adverse events were infusion reactions (82 [46%] patients in the isatuximab group and four [3%] in the control group) and upper respiratory tract infections (71 [40%] and 34 [28%], respectively). Discontinuations due to treatment-emergent adverse events were similar between treatment groups (24 [14%] in the isatuximab group and 22 [18%] in the control group), despite an additional 30 weeks of exposure in the isatuximab group. 12 (7%) patients in the isatuximab group and six (5%) patients in the control group had a treatment-related adverse event with a fatal outcome during study treatment.

Interpretation: At the time of the current analysis, a difference in overall survival could not be detected between the treatment groups, and no new safety signals were observed. Collectively, the evidence suggests that isatuximab plus carfilzomib-dexamethasone is a key treatment for patients with relapsed or refractory multiple myeloma.

Funding: Sanofi.

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来源期刊
Lancet Haematology
Lancet Haematology HEMATOLOGY-
CiteScore
26.00
自引率
0.80%
发文量
323
期刊介绍: Launched in autumn 2014, The Lancet Haematology is part of the Lancet specialty journals, exclusively available online. This monthly journal is committed to publishing original research that not only sheds light on haematological clinical practice but also advocates for change within the field. Aligned with the Lancet journals' tradition of high-impact research, The Lancet Haematology aspires to achieve a similar standing and reputation within its discipline. It upholds the rigorous reporting standards characteristic of all Lancet titles, ensuring a consistent commitment to quality in its contributions to the field of haematology.
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