Long-term Survival Update and Extended RAS Mutational Analysis of the CAIRO2 Trial: Addition of Cetuximab to CAPOX/Bevacizumab in Metastatic Colorectal Cancer

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2023-03-01 DOI:10.1016/j.clcc.2022.11.006
Sanne ten Hoorn , Linda Mol , Dirkje W. Sommeijer , Lisanne Nijman , Tom van den Bosch , Tim R. de Back , Bauke Ylstra , Erik van Dijk , Carel J.M. van Noesel , Roy J. Reinten , Iris D. Nagtegaal , Miriam Koopman , Cornelis J.A. Punt , Louis Vermeulen
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引用次数: 1

Abstract

Background

Here we present updated survival of the CAIRO2 trial and assessed whether the addition of anti-EGFR to anti-VEGF therapy could still be an effective treatment option for patients with extended RAS/BRAF wildtype and left-sided metastatic colorectal cancer (mCRC).

Materials and Methods

Retrospective updated survival and extended RAS and BRAF V600E mutational analysis were performed in the CAIRO2 trial, a multicenter, randomized phase III trial on the effect of adding cetuximab to a combination of capecitabine, oxaliplatin (CAPOX), and bevacizumab in mCRC.

Results

Updated survival analysis confirmed that the addition of cetuximab did not provide a benefit on either progression free (PFS) or overall survival (OS) in the intention-to-treat population. With the extended mutational analyses 31 KRAS, 31 NRAS and 12 BRAF V600E additional mutations were found. No benefit of the addition of cetuximab was observed within the extended wildtype group, even when selecting only left-sided tumors (PFS HR 0.96, p = 0.7775). However, compared to the original trial an increase of 6.5 months was seen for patients with both extended wildtype and left-sided tumors (median OS 28.6 months).

Conclusion

Adding cetuximab to CAPOX and bevacizumab does not provide clinical benefit in patients with mCRC, even in the extended wildtype group with left-sided tumors. However, in the extended wildtype group we did observe clinically relevant higher survival compared to the initial trial report, indicating that it is important to analyze a broader panel of RAS and BRAF variants using more recent sequencing techniques when assessing survival benefit after anti-EGFR therapy.

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CAIRO2试验的长期生存更新和扩展RAS突变分析:在转移性结直肠癌癌症的CAPOX/贝伐单抗中添加西妥昔单抗
背景我们介绍了CAIRO2试验的最新生存率,并评估了在抗血管内皮生长因子治疗中添加抗EGFR是否仍然是延长RAS/BRAF野生型和左侧转移性癌症(mCRC)患者的有效治疗选择CAIRO2试验,一项关于在卡培他滨、奥沙利铂(CAPOX)和贝伐单抗的组合中添加西妥昔单抗对mCRC的影响的多中心随机III期试验。结果更新的生存分析证实,在意向治疗人群中,添加西妥单抗对无进展(PFS)或总生存期(OS)没有益处。通过扩展突变分析,发现了31个KRAS、31个NRAS和12个BRAF V600E的额外突变。在扩展野生型组中,即使只选择左侧肿瘤,也没有观察到添加西妥昔单抗的益处(PFS HR 0.96,p=0.7775)。然而,与最初的试验相比,患有扩展型野生型和左侧肿瘤的患者增加了6.5个月(中位OS 28.6个月)。结论在CAPOX和贝伐单抗的基础上添加西妥昔单抗对mCRC患者没有临床益处,即使在患有左侧肿瘤的扩展野生型组中也是如此。然而,与最初的试验报告相比,在扩展野生型组中,我们确实观察到了临床相关的更高生存率,这表明在评估抗EGFR治疗后的生存益处时,使用更新的测序技术分析更广泛的RAS和BRAF变体是很重要的。
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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