Efficacy of Regorafenib and Trifluridine/Tipiracil According to Extended RAS Evaluation in Advanced Metastatic Colorectal Cancer Patients: A Multicenter Retrospective Analysis

IF 4.4 3区 医学 Q2 ONCOLOGY Targeted Oncology Pub Date : 2024-04-13 DOI:10.1007/s11523-024-01050-3
Michele Basso, Carlo Signorelli, Maria Alessandra Calegari, Jessica Lucchetti, Ina Valeria Zurlo, Emanuela Dell’Aquila, Giulia Arrivi, Federica Zoratto, Fiorenza Santamaria, Rosa Saltarelli, Giovanni Trovato, Giulia Caira, Lorenzo Angotti, Marta Schirripa, Annunziato Anghelone, Francesco Schietroma, Mario Giovanni Chilelli, Lisa Salvatore, Carmelo Pozzo, Giampaolo Tortora
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Abstract

Background

There are few molecular markers driving treatment selection in later lines of treatment for advanced colorectal cancer patients. The vast majority of patients who progress after first- and second-line therapy undergo chemotherapy regardless of molecular data.

Objective

We aimed to assess the prognostic and predictive effects of specific RAS mutations on overall survival of patients receiving regorafenib (rego), trifluridine/tipiracil (TFD/TPI), or both.

Patients and methods

This was a retrospective observational study based on data from a previous study of our research network, involving nine Italian institutions over a 10-year timeframe (2012–2022). Extended RAS analysis, involving KRAS exon 2–4 and NRAS exon 2–4, and BRAF were the main criteria for inclusion in this retrospective evaluation. Patients with BRAF mutation were excluded. Patients were classified according to treatment (rego- or TFD/TPI-treated) and RAS mutational status (wild-type [WT], KRAS codon 12 mutations, KRAS codon 13 mutations, KRAS rare mutations and NRAS mutations, KRAS G12C mutation and KRAS G12D mutation).

Results

Overall, 582 patients were included in the present analysis. Overall survival did not significantly differ in rego-treated patients according to RAS extended analysis, although a trend toward a better median survival in patients carrying G12D mutation (12.0 months), Codon 13 mutation (8.0 months), and Codon 12 mutation (7.0 months) has been observed, when compared with WT patients (6.0 months). Overall survival did not significantly differ in TFD/TPI-treated patients according to RAS extended analysis, although a trend toward a better median survival in WT patients had been observed (9.0 months) in comparison with the entire population (7.0 months). Patients receiving both drugs displayed a longer survival when compared with the population of patients receiving rego alone (p = 0.005) as well as the population receiving TFD/TPI alone (p < 0.001), suggesting a group enriched for favorable prognostic factors. However, when each group was analyzed separately, the addition of TFD/TPI therapy to the rego-treated group improved survival only in all-RAS WT patients (p = 0.003). Differently, the addition of rego therapy to TFD/TPI-treated patients significantly improved OS in the Codon 12 group (p = 0.0004), G12D group (p = 0.003), and the rare mutations group (p = 0.02), in addition to all-RAS WT patients (p = 0.002). The rego-TFD/TPI sequence, compared with the reverse sequence, significantly improved OS only in the KRAS codon 12 group (p = 0.003).

Conclusions

Our data demonstrate that RAS mutations do not affect outcome in rego-treated patients as well as TFD/TPI-treated patients. Nevertheless, a trend toward a higher efficacy of rego in RAS-mutated (in particular codon 12, rare RAS mutations, and G12D) patients has been recorded. The rego-TFD/TPI sequence seems to be superior to the reverse sequence in patients carrying an RAS codon 12 mutation, although the impact of other factors as disease burden or performance status cannot be excluded.

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晚期转移性结直肠癌患者的瑞戈非尼和曲氟脲苷/替吡拉西根据扩展 RAS 评估的疗效:多中心回顾性分析
背景在晚期结直肠癌患者的后期治疗中,几乎没有分子标记物可以驱动治疗选择。我们旨在评估特定 RAS 基因突变对接受瑞戈非尼 (rego)、三氟啶/替吡嘧啶 (TFD/TPI) 或同时接受这三种治疗的患者总生存期的预后和预测作用。患者和方法这是一项回顾性观察研究,基于我们研究网络之前的一项研究数据,涉及 9 家意大利机构,历时 10 年(2012-2022 年)。本次回顾性评估的主要纳入标准是扩展 RAS 分析(包括 KRAS 2-4 外显子和 NRAS 2-4 外显子)和 BRAF。BRAF突变的患者被排除在外。根据治疗方法(rego或TFD/TPI治疗)和RAS突变状态(野生型[WT]、KRAS第12密码子突变、KRAS第13密码子突变、KRAS罕见突变和NRAS突变、KRAS G12C突变和KRAS G12D突变)对患者进行分类。尽管与 WT 患者(6.0 个月)相比,G12D 突变(12.0 个月)、13 号密码子突变(8.0 个月)和 12 号密码子突变(7.0 个月)患者的中位生存期有提高的趋势,但根据 RAS 扩展分析,Rego 治疗患者的总生存期没有明显差异。根据 RAS 扩展分析,TFD/TPI 治疗患者的总生存期没有明显差异,但观察到 WT 患者的中位生存期(9.0 个月)与整个人群(7.0 个月)相比有更好的趋势。与单独接受雷戈治疗的患者(p = 0.005)和单独接受 TFD/TPI 治疗的患者(p <0.001)相比,接受两种药物治疗的患者生存期更长,这表明该组患者富含有利的预后因素。然而,当对每组患者进行单独分析时,在雷戈治疗组中增加 TFD/TPI 治疗仅能改善全 RAS WT 患者的生存率(p = 0.003)。与此不同的是,在TFD/TPI治疗患者的基础上加用rego治疗可显著改善Codon 12组(p = 0.0004)、G12D组(p = 0.003)和罕见突变组(p = 0.02)的OS,此外还可改善所有RAS WT患者的OS(p = 0.002)。结论我们的数据表明,RAS突变不会影响Rego治疗患者和TFD/TPI治疗患者的预后。然而,RAS突变(尤其是密码子12、罕见RAS突变和G12D)患者的疗效有提高的趋势。对于携带RAS第12密码子突变的患者,rego-TFD/TPI序列似乎优于反向序列,但不能排除疾病负担或表现状态等其他因素的影响。
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
Targeted Oncology
Targeted Oncology 医学-肿瘤学
CiteScore
8.40
自引率
3.70%
发文量
64
审稿时长
>12 weeks
期刊介绍: Targeted Oncology addresses physicians and scientists committed to oncology and cancer research by providing a programme of articles on molecularly targeted pharmacotherapy in oncology. The journal includes: Original Research Articles on all aspects of molecularly targeted agents for the treatment of cancer, including immune checkpoint inhibitors and related approaches. Comprehensive narrative Review Articles and shorter Leading Articles discussing relevant clinically established as well as emerging agents and pathways. Current Opinion articles that place interesting areas in perspective. Therapy in Practice articles that provide a guide to the optimum management of a condition and highlight practical, clinically relevant considerations and recommendations. Systematic Reviews that use explicit, systematic methods as outlined by the PRISMA statement. Adis Drug Reviews of the properties and place in therapy of both newer and established targeted drugs in oncology.
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