ROCKET: Phase II Randomized, Active-controlled, Multicenter Trial to Assess the Safety and Efficacy of RRx-001 + Irinotecan vs. Single-agent Regorafenib in Third/Fourth Line Colorectal Cancer

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Tony R. Reid , Nacer Abrouk , Scott Caroen , Bryan Oronsky , Meaghan Stirn , Christopher Larson , Keola Beale , Susan J. Knox , George Fisher
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引用次数: 3

Abstract

Introduction

RRx-001 is a novel cysteine-targeted alkylating agent that releases nitric oxide (NO). The primary biological activities of this hybrid molecule include macrophage repolarizing and vascular normalization. The purpose of this clinical trial (ROCKET) (NCT02096354) was to compare the safety and efficacy of the combination therapy RRx-001 + irinotecan vs. regorafenib in third/fourth line colorectal cancer that previously received treatment with irinotecan.

Patients and Methods

A total of 34 patients were randomized (24 to RRx-001 + irinotecan (RxI) and 10 to single-agent regorafenib (RegI)) and were the basis for the intention-to-treat analysis (ITT, comprising all 34 patients). RRx-001 treatment was administered as an up-to-2-month “primer” followed by irinotecan for patients randomized to the RRx-001 arm (24). The efficacy and safety data are presented for the 34 patients in the (ITT) efficacy analysis. Therapy consisted of intravenous administration of RRx-001 at 4 mg once weekly for up to 2 months, at which point RRx-001 was discontinued, followed by intravenous infusion of irinotecan at 180 mg/m2 on day 1 in a 21-day cycle vs. 160 mg oral regorafenib daily for 3/4 weeks followed at progression, if applicable, by irinotecan 180 mg/m2 on day 1 in a 21-day cycle. There were 3 patients (3/24 = 12.5%) with prior single agent irinotecan on the RRx-001 randomized arm and 2 (2/10 = 20%) on the regorafenib randomized arm. Numerous patients had irinotecan combination therapies prior to randomized treatment. There were 15 patients on RRx-001 arm that received irinotecan post-RRx-001 in the randomized trial. There were 5 PRs on RRx-001 plus irinotecan leading to an overall response of 20.8% (5/24). There were 37.5% (9/24) of RRx-001 randomized patients with KRAS mutant type while 60% (6/10) regorafenib randomized patients were of KRAS type mutant. There were only 4 patients with available QOL and Edmonton Symptom Assessment System, an insufficient sample size to allow for any meaningful analysis.

Results

Median patient follow-up was approximately 14.5 months (SD 4.5 months). Median overall survival was 8.6 months for RxI and 4.7 months for RegI. Median progression free survival was 6.1 months for RxI vs. 1.7 months for RegI (a statistically significant result, 2-sided log-rank test, P = .0030). The toxicity profile of RxI was substantially improved compared with RegI.

Conclusion

The results of this trial demonstrate improved efficacy of RxI compared with RegI in patients with metastatic colorectal cancer after previous treatment with irinotecan, and late-stage clinical development in this indication is planned on the strength of the observed “signal” accompanied by a sufficient safety profile.

ROCKET:第二阶段随机、活性对照、多中心试验,评估RRx-001+伊立替康与单剂量雷戈非尼治疗三/四线结直肠癌癌症的安全性和有效性
引言RRx-001是一种新型的半胱氨酸靶向烷基化剂,可释放一氧化氮(NO)。这种杂交分子的主要生物学活性包括巨噬细胞复极和血管正常化。本临床试验(ROCKET)(NCT02096354)的目的是比较RRx-001+伊立替康与瑞戈非尼联合治疗先前接受伊立替康治疗的三/四线癌症的安全性和有效性。患者和方法共有34名患者被随机分组(24名患者接受RRx-001+伊立替康(RxI)治疗,10名患者接受单剂瑞戈非尼(RegI)治疗),这是意向治疗分析(ITT,包括所有34名患者)的基础。RRx-001治疗作为长达2个月的“引物”,随后对随机分配到RRx-001组的患者进行伊立替康治疗(24)。34名患者的疗效和安全性数据显示在(ITT)疗效分析中。治疗包括静脉注射RRx-001,每周一次,每次4 mg,持续2个月,此时RRx-001停止,然后在21天周期的第1天静脉输注180 mg/m2的伊立替康,而口服雷戈非尼,每天160 mg,持续3/4周,如果适用,在进展时,在21天循环的第1天依立替康180 mg/m2。RRx-001随机组中有3名患者(3/24=12.5%)既往使用过单剂伊立替康,雷戈非尼随机组中则有2名患者(2/10=20%)。许多患者在随机治疗前接受了伊立替康联合治疗。在随机试验中,RRx-001组有15名患者在RRx-001后接受了伊立替康治疗。RRx-001加伊立替康共有5例PR,总有效率为20.8%(5/24)。有37.5%(9/24)的RRx-001随机患者为KRAS突变型,而60%(6/10)的雷戈非尼随机患者为KRAS突变型。只有4名患者具有可用的生活质量和埃德蒙顿症状评估系统,样本量不足,无法进行任何有意义的分析。结果患者中位随访时间约14.5个月(SD 4.5个月)。RxI和RegI的中位总生存期分别为8.6个月和4.7个月。RxI的中位无进展生存期为6.1个月,RegI为1.7个月(具有统计学意义的结果,双侧对数秩检验,P=0.030)。与RegI相比,RxI毒性显著改善。结论本试验的结果表明,与RegI相比,RxI在既往伊立替康治疗转移性结直肠癌癌症患者中的疗效有所改善,该适应症的后期临床发展计划基于观察到的“信号”强度和足够的安全性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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