对输血依赖型低危骨髓增生异常综合征（LR-MDS）的红细胞生成刺激剂（ESA）无效患者使用 Luspatercept 与 Epoetin alfa 的疗效和安全性：COMMAND 试验的全面分析

IF 0.7 Q4 HEMATOLOGY

Leukemia Research Reports Pub Date : 2024-01-01 DOI:10.1016/j.lrr.2024.100447

G. Garcia-Manero , U. Platzbecker , V. Santini , A. Zeidan , P. Fenaux , R. Komrokji , J. Shortt , D. Valcarcel , A. Jonasova , S. Dimicoli-Salazar , I.S. Tiong , C.-C. Lin , J. Li , J. Zhang , A.C. Giuseppi , S. Kreitz , V. Pozharskaya , K. Keeperman , S. Rose , T. Prebet , M. Della Porta

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引用次数: 0

摘要

方法363名患者（年龄≥18岁，输血依赖型LR-MDS，血清促红细胞生成素<500 U/L）按1:1随机分配到luspatercept或EA。主要终点是实现红细胞输血独立（RBC-TI）≥12 wk，同时平均血红蛋白增加≥1.5 g/dL（第1-24周）。次要终点包括RBC-TI≥12和24周、血液学改善-红细胞（HI-E）≥8周（第1-24周）、RBC-TI≥12周持续时间和安全性。结果截至2023年3月31日，110/182（60.4%）名接受Luspatercept治疗的患者与63/181（34.8%）名接受EA治疗的患者达到了主要终点（P<0.0001）。在包括地区在内的大多数亚组中，Luspatercept更有利于达到主要终点。luspatercept与EA的中位治疗时间（范围）分别为51.3（3-196）周和37.0（1-202）周。分别有68.1%和48.6%接受过luspatercept与EA治疗的患者达到了RBC-TI≥12周；分别有47.8%和30.9%的患者达到了RBC-TI 24周；分别有74.4%和53.0%的患者达到了HI-E≥8周。RBC-TI≥12周的中位持续时间（95% CI）为：Luspatercept为128.1周（108.3-无法估计[NE]），EA为89.7周（55.9-157.3）（HR，0.534；图）。在接受luspatercept和EA治疗的患者中，分别有2.7%和3.3%的患者进展为急性髓细胞性白血病；分别有97.8%和92.2%的患者报告了任何级别的治疗突发不良事件（TEAEs）；分别有58.5%和49.2%的患者报告了3/4级TEAEs。治疗期间和治疗后的死亡率在两组间相似。结论Luspatercept的RBC-TI持续时间和红细胞反应优于EA。Luspatercept的安全性结果与之前的MDS研究结果一致。

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EFFICACY AND SAFETY OF LUSPATERCEPT VERSUS EPOETIN ALFA IN ERYTHROPOIESIS-STIMULATING AGENT (ESA)-NAIVE PATIENTS WITH TRANSFUSION-DEPENDENT LOWER-RISK MYELODYSPLASTIC SYNDROMES (LR-MDS): FULL ANALYSIS OF THE COMMANDS TRIAL

Introduction

We report the full analysis of the COMMANDS trial assessing efficacy and safety of luspatercept versus epoetin alfa (EA) in ESA-naive patients with LR-MDS.

Methods

363 patients (aged ≥18 y, with transfusion-dependent LR-MDS, serum erythropoietin <500 U/L) were randomized 1:1 to luspatercept or EA. Primary endpoint was achievement of red blood cell transfusion independence (RBC-TI) ≥12 wk with concurrent mean hemoglobin increase ≥1.5 g/dL (wk 1–24). Secondary endpoints included achievement of RBC-TI ≥12 and 24 wk, hematologic improvement–erythroid (HI-E) ≥8 wk (wk 1–24), RBC-TI ≥12 wk duration, and safety.

Results

As of 31Mar2023, 110/182 (60.4%) luspatercept-treated versus 63/181 (34.8%) EA-treated patients achieved the primary endpoint (P<0.0001). Primary endpoint achievement favored luspatercept in most subgroups including region. Median (range) treatment duration was 51.3 (3–196) and 37.0 (1–202) wk for luspatercept versus EA. 68.1% and 48.6% of luspatercept- versus EA-treated patients, respectively, achieved RBC-TI ≥12 wk; 47.8% and 30.9% achieved RBC-TI 24 wk; 74.4% and 53.0% achieved HI-E ≥8 wk. Median (95% CI) duration of RBC-TI ≥12 wk was 128.1 wk (108.3–not estimable [NE]) with luspatercept versus 89.7 wk (55.9–157.3) with EA (HR, 0.534; Figure). 2.7% and 3.3% of luspatercept- and EA-treated patients, respectively, progressed to AML; 97.8% and 92.2% reported any-grade treatment-emergent adverse events (TEAEs); 58.5% and 49.2% reported grade 3/4 TEAEs. Death rates on- and post-treatment were similar between arms.

Conclusions

RBC-TI duration and erythroid responses achieved with luspatercept were superior to EA. Luspatercept safety results were consistent with previous MDS studies.

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来源期刊

Leukemia Research Reports Medicine-Oncology

CiteScore

1.70

自引率

0.00%

发文量

审稿时长

23 weeks