First-Line Systemic Treatment for Initially Unresectable Colorectal Liver Metastases: Post Hoc Analysis of the CAIRO5 Randomized Clinical Trial.

IF 28.4 1区医学 Q1 Biochemistry, Genetics and Molecular Biology Jama Oncology Pub Date : 2024-11-21 DOI:10.1001/jamaoncol.2024.5174

Marinde J G Bond, Karen Bolhuis, Olaf J L Loosveld, Jan Willem B de Groot, Helga Droogendijk, Helgi H Helgason, Mathijs P Hendriks, Joost M Klaase, Geert Kazemier, Mike S L Liem, Arjen M Rijken, Cornelis Verhoef, Johannes H W de Wilt, Koert P de Jong, Michael F Gerhards, Martinus J van Amerongen, Marc R W Engelbrecht, Krijn P van Lienden, John J Hermans, I Quintus Molenaar, Dirk J Grünhagen, Bart de Valk, Brigitte C M Haberkorn, Emile D Kerver, Frans Erdkamp, Robbert J van Alphen, Daniëlle Mathijssen-van Stein, Aysun Komurcu, Anne M May, Rutger-Jan Swijnenburg, Cornelis J A Punt

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Abstract

Importance: In patients with colorectal cancer and unresectable liver-only metastases (CRLM), treatment with folinic acid, fluorouracil, and oxaliplatin (FOLFOX) plus irinotecan (FOLFOXIRI) and bevacizumab vs FOLFOX/folinic acid, fluorouracil, and irinotecan (FOLFIRI) plus bevacizumab increased progression-free survival, response, and R0/R1 resection/ablation rates, as well as toxic effects in RAS/BRAFV600E-variant and/or right-sided tumors. FOLFOX/FOLFIRI-panitumumab vs FOLFOX/FOLFIRI-bevacizumab increased response at the cost of more toxic effects in RAS/BRAFV600E wild-type, left-sided tumors.

Objective: To present long-term outcomes of treatment with FOLFOXIRI plus bevacizumab vs FOLFOX/FOLFIRI plus bevacizumab and FOLFOX/FOLFIRI plus panitumumab vs FOLFOX/FOLFIRI + bevacizumab.

Design, setting, and participants: The randomized phase 3 CAIRO5 trial included patients with initially unresectable CRLM in 46 Dutch centers and 1 Belgian center between November 2014 and January 2022. A liver expert panel repeatedly evaluated resectability.

Intervention: Patients with RAS/BRAFV600E-variant and/or right-sided tumors randomly received FOLFOX/FOLFIRI-bevacizumab (group 1) or FOLFOXIRI-bevacizumab (group 2), and those with RAS/BRAFV600E wild-type, left-sided tumors received FOLFOX/FOLFIRI-bevacizumab (group 3) or FOLFOX/FOLFIRI-panitumumab (group 4). Adjuvant chemotherapy (ACT) after complete local treatment was recommended but not standard.

Main outcomes and measures: Overall survival (OS) was analyzed as a secondary outcome. Other outcomes were post hoc analyses.

Results: A total of 530 patients (327 male [62%] and 203 female individuals [38%]; median age, 62 [IQR, 54-69] years) were randomized: 148 in group 1, 146 in group 2, 118 in group 3, and 118 in group 4. The median OS in group 1 was 23.6 (95% CI, 20.1-27.5) vs 24.1 (95% CI, 21.0-30.9) months in group 2 (hazard ratio [HR], 0.90; 95% CI, 0.70-1.17; P = .44), and 39.9 (95% CI, 30.7-44.6) in group 3 vs 38.3 (95% CI, 35.3-51.3) months in group 4 (HR, 0.95; 95% CI, 0.68-1.32; P = .75). OS was longest after complete local treatment without early (≤6 months) recurrence (64.3 months; 95% CI, 57.6 to not reached) and salvage local treatment options after early recurrence (58.9; 95% CI, 47.3 to not reached), followed by patients without salvage local treatment after early recurrence (30.5; 95% CI, 24.4-33.4) and with incomplete local treatment (28.7; 95% CI, 25.9-38.3), and worst in patients with continued unresectability (18.3; 95% CI, 15.7-20.0). After confounder adjustment, ACT was associated with longer OS (HR, 0.66; 95% CI, 0.44-0.98) and relapse-free survival (HR, 0.65; 95% CI, 0.48-0.88) and less early recurrence without salvage local treatment (odds ratio, 0.46; 95% CI, 0.25-0.85).

Conclusions and relevance: These results support using FOLFOX/FOLFIRI-bevacizumab for patients with initially unresectable CRLM irrespective of RAS/BRAFV600E status and tumor sidedness. Patients with complete local liver treatment with salvage local treatment in case of early recurrence had the longest OS. ACT might be considered for these patients.

Trial registration: ClinicalTrials.gov NCT02162563.

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最初无法切除的结直肠肝转移的一线系统治疗：CAIRO5 随机临床试验的事后分析。

重要性：在结直肠癌和不可切除肝转移灶（CRLM）患者中，亚叶酸、氟尿嘧啶和奥沙利铂（FOLFOX）加伊立替康（FOLFOXIRI）和贝伐珠单抗治疗与FOLFOX/亚叶酸、氟尿嘧啶和伊立替康（FOLFOXIRI）加贝伐珠单抗治疗相比，无进展生存期、反应和R0/R1切除/消融率均有所提高、氟尿嘧啶和伊立替康（FOLFIRI）加贝伐珠单抗可提高 RAS/BRAFV600E 变异和/或右侧肿瘤患者的无进展生存期、反应和 R0/R1 切除/消融率以及毒性反应。FOLFOX/FOLFIRI-帕尼单抗与FOLFOX/FOLFIRI-贝伐单抗相比，在RAS/BRAFV600E野生型、左侧肿瘤中，反应增加的代价是毒性反应增加：介绍FOLFOXIRI加贝伐单抗与FOLFOX/FOLFIRI加贝伐单抗、FOLFOX/FOLFIRI加帕尼单抗与FOLFOX/FOLFIRI+贝伐单抗治疗的长期疗效：随机3期CAIRO5试验纳入了2014年11月至2022年1月期间在46个荷兰中心和1个比利时中心接受治疗的最初无法切除的CRLM患者。肝脏专家小组反复评估可切除性：RAS/BRAFV600E变异型和/或右侧肿瘤患者随机接受FOLFOX/FOLFIRI-贝伐单抗（第1组）或FOLFOXIRI-贝伐单抗（第2组）治疗，RAS/BRAFV600E野生型左侧肿瘤患者接受FOLFOX/FOLFIRI-贝伐单抗（第3组）或FOLFOX/FOLFIRI-帕尼单抗（第4组）治疗。建议在完成局部治疗后进行辅助化疗（ACT），但这不是标准疗法：总生存期（OS）作为次要结果进行分析。其他结果均为事后分析：共有 530 名患者（327 名男性[62%]，203 名女性[38%]；中位年龄 62 [IQR, 54-69] 岁）接受了随机治疗：第 1 组的中位 OS 为 23.6 个月（95% CI，20.1-27.5），第 2 组为 24.1 个月（95% CI，21.0-30.9）（危险比 [HR]，0.90；95% CI，0.70-1.17；P = .44），第 3 组为 39.9（95% CI，30.7-44.6）个月，第 4 组为 38.3（95% CI，35.3-51.3）个月（HR，0.95；95% CI，0.68-1.32；P = .75）。完全局部治疗后无早期（≤6 个月）复发（64.3 个月；95% CI，57.6 至未达到）和早期复发后挽救性局部治疗方案的 OS 最长（58.9；95% CI，47.其次是早期复发后未进行挽救性局部治疗的患者（30.5；95% CI，24.4-33.4）和局部治疗不完全的患者（28.7；95% CI，25.9-38.3），最差的是持续无法切除的患者（18.3；95% CI，15.7-20.0）。经混杂因素调整后，ACT与较长的OS（HR，0.66；95% CI，0.44-0.98）和无复发生存期（HR，0.65；95% CI，0.48-0.88）相关，且在未进行挽救性局部治疗的情况下，早期复发率较低（几率比，0.46；95% CI，0.25-0.85）：这些结果支持对最初无法切除的CRLM患者使用FOLFOX/FOLFIRI-贝伐单抗治疗，而不论RAS/BRAFV600E状态和肿瘤侧切情况。完全肝脏局部治疗并在早期复发时进行挽救性局部治疗的患者的OS最长。这些患者可考虑进行ACT治疗：试验注册：ClinicalTrials.gov NCT02162563。

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来源期刊

Jama Oncology Medicine-Oncology

CiteScore

37.50

自引率

1.80%

发文量

423

期刊介绍： At JAMA Oncology, our primary goal is to contribute to the advancement of oncology research and enhance patient care. As a leading journal in the field, we strive to publish influential original research, opinions, and reviews that push the boundaries of oncology science. Our mission is to serve as the definitive resource for scientists, clinicians, and trainees in oncology globally. Through our innovative and timely scientific and educational content, we aim to provide a comprehensive understanding of cancer pathogenesis and the latest treatment advancements to our readers. We are dedicated to effectively disseminating the findings of significant clinical research, major scientific breakthroughs, actionable discoveries, and state-of-the-art treatment pathways to the oncology community. Our ultimate objective is to facilitate the translation of new knowledge into tangible clinical benefits for individuals living with and surviving cancer.

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