Sequential RAS mutations evaluation in cell-free DNA of patients with tissue RAS wild-type metastatic colorectal cancer: the PERSEIDA (Cohort 2) study.

IF 2.8 3区医学 Q2 ONCOLOGY

Clinical & Translational Oncology Pub Date : 2024-10-01 Epub Date: 2024-04-20 DOI:10.1007/s12094-024-03487-4

Manuel Valladares-Ayerbes, Maria José Safont, Encarnación González Flores, Pilar García-Alfonso, Enrique Aranda, Ana-Maria López Muñoz, Esther Falcó Ferrer, Luís Cirera Nogueras, Nuria Rodríguez-Salas, Jorge Aparicio, Marta Llanos Muñoz, Paola Patricia Pimentel Cáceres, Oscar Alfredo Castillo Trujillo, Rosario Vidal Tocino, Mercedes Salgado Fernández, Antonieta Salud-Salvia, Bartomeu Massuti Sureda, Rocio Garcia-Carbonero, Maria Ángeles Vicente Conesa, Ariadna Lloansí Vila

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引用次数: 0

Abstract

Purpose: RAS (KRAS/NRAS) mutational status on a tumor biopsy is mandatory to guide the best treatment in metastatic colorectal cancer (mCRC). Determining the RAS mutational status by tumor-tissue biopsy is essential in guiding the optimal treatment decision for mCRC. RAS mutations are negative predictive factors for the use of EGFR monoclonal antibodies. Cell-free DNA (cfDNA) analysis enables minimally invasive monitoring of tumor evolution.

Methods/patients: PERSEIDA was an observational, prospective study assessing cfDNA RAS, BRAF and EGFR mutations (using Idylla™) in first-line mCRC, RAS wild-type (baseline tumor-tissue biopsy) patients (cohort 2). Plasma samples were collected before first-line treatment, after 20 ± 2 weeks, and at disease progression.

Results: 117 patients were included (103 received panitumumab + chemotherapy as first-line treatment). At baseline, 7 (6.8%) patients had RAS mutations, 4 (3.9%) BRAF mutations and no EGFR mutations were detected (cfDNA, panitumumab + chemotherapy subpopulation [panitumumab + Ch]). The baseline RAS mutational status concordance between tissue and liquid biopsies was 94.0% (93.2%, panitumumab + Ch). At 20 weeks, only one patient in the study (included in the panitumumab + Ch) had an emerging cfDNA RAS mutation. No emerging BRAF or EGFR mutations were reported. At disease progression, 6 patients had emergent mutations not present at baseline (RAS conversion rate: 13.3% [6/45]; 15.0% [6/40], panitumumab + Ch).

Conclusions: The concordance rate between liquid and solid biopsies at baseline was very high, as previously reported, while our results suggest a considerable emergence of RAS mutations during disease progression. Thus, the dynamics of the genomic landscape in ctDNA may provide relevant information for the management of mCRC patients.

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组织 RAS 野生型转移性结直肠癌患者无细胞 DNA 中 RAS 序列突变评估：PERSEIDA（队列 2）研究。

目的：肿瘤活检的 RAS（KRAS/NRAS）突变状态是指导转移性结直肠癌（mCRC）最佳治疗的必要条件。通过肿瘤组织活检确定 RAS 突变状态对于指导 mCRC 的最佳治疗决策至关重要。RAS 突变是使用表皮生长因子受体单克隆抗体的阴性预测因素。无细胞DNA（cfDNA）分析可实现肿瘤演变的微创监测：PERSEIDA是一项前瞻性观察研究，评估一线mCRC、RAS野生型（基线肿瘤组织活检）患者（队列2）的cfDNA RAS、BRAF和表皮生长因子受体突变（使用Idylla™）。在一线治疗前、20 ± 2 周后和疾病进展时采集血浆样本：共纳入 117 例患者（其中 103 例接受了帕尼单抗+化疗作为一线治疗）。基线时，7 例（6.8%）患者出现 RAS 突变，4 例（3.9%）出现 BRAF 突变，未检测到表皮生长因子受体突变（cfDNA，帕尼单抗 + 化疗亚群 [panitumumab + Ch]）。组织活检和液体活检的基线 RAS 突变状态一致性为 94.0%（93.2%，帕尼单抗 + Ch）。20周时，研究中只有一名患者（包括帕尼单抗+ Ch）出现了新的cfDNA RAS突变。没有报告出现 BRAF 或 EGFR 突变。疾病进展时，6 名患者出现了基线时未出现的突变（RAS 转换率：13.3% [6/45]；15.0% [6/40]，帕尼单抗 + Ch）：结论：与之前的报道一样，基线时液体活检和实体活检的一致性非常高，而我们的结果表明，在疾病进展过程中出现了相当多的 RAS 突变。因此，ctDNA中基因组的动态变化可为mCRC患者的治疗提供相关信息。

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

Clinical & Translational Oncology 医学-肿瘤学

CiteScore

6.20

自引率

2.90%

发文量

240

审稿时长

1 months

期刊介绍： Clinical and Translational Oncology is an international journal devoted to fostering interaction between experimental and clinical oncology. It covers all aspects of research on cancer, from the more basic discoveries dealing with both cell and molecular biology of tumour cells, to the most advanced clinical assays of conventional and new drugs. In addition, the journal has a strong commitment to facilitating the transfer of knowledge from the basic laboratory to the clinical practice, with the publication of educational series devoted to closing the gap between molecular and clinical oncologists. Molecular biology of tumours, identification of new targets for cancer therapy, and new technologies for research and treatment of cancer are the major themes covered by the educational series. Full research articles on a broad spectrum of subjects, including the molecular and cellular bases of disease, aetiology, pathophysiology, pathology, epidemiology, clinical features, and the diagnosis, prognosis and treatment of cancer, will be considered for publication.