转移性结直肠癌中循环肿瘤DNA从一线治疗到后续治疗的新RAS-WT演变
Evolution of Neo-RAS-WT in Circulating Tumor DNA from First-Line to Subsequent Therapies in Metastatic Colorectal Cancer.
作者信息
Siringo Marco, De Meo Michela, Bottillo Irene, Grammatico Paola, Cortesi Enrico, Nicolazzo Chiara, Gazzaniga Paola
机构信息
Department of Molecular Medicine, Sapienza University of Rome, 00185 Rome, Italy.
Division of Medical Genetics, Department of Experimental Medicine, San Camillo-Forlanini Hospital, Sapienza University, 00185 Rome, Italy.
出版信息
Cancers (Basel). 2025 Mar 22;17(7):1070. doi: 10.3390/cancers17071070.
: In metastatic colorectal cancer (mCRC), liquid biopsy has enabled the identification of "neo-RAS-Wild-Type (WT)", a transient phase characterized by the disappearance of RAS mutations, with significant clinical implications for re-sensitization to EGFR blockade. This study aimed to prospectively track the kinetics of neo-RAS-WT in circulating tumor DNA (ctDNA) among RAS-mutant mCRC patients receiving first-line and subsequent systemic therapies. : A total of 380 serial blood samples from 35 patients were analyzed. Each patient provided a median of 10 ctDNA samples at three-month intervals during first-line and subsequent therapies. The patients were categorized into three groups: neo-RAS-WT, non-shedding, and persistent mutant. : During first-line treatment, 68% of patients transitioned to RAS-WT. Of these, 17% were neo-RAS-WT, while the majority were classified as non-shedding. In the second-line setting, the percentage of neo-RAS-WT increased to 34%, which dropped to 8.5% during the third-line setting. The duration of the neo-RAS-WT window was significantly longer in neo-RAS-WT patients compared to non-shedding patients ( = 0.037). Patients who achieved RAS-WT status had improved progression-free survival (PFS) compared to those with persistent mutant, with significant differences observed across all treatment lines: first-line ( = 0.004), second-line ( < 0.0001), and third-line ( = 0.001). Multivariate analysis revealed that the duration of the RAS-WT window correlated with extended first-line PFS (HR: 0.78; 95% CI: 0.69-0.89; < 0.0001), second-line PFS (HR: 0.66; 95% CI: 0.52-0.84; = 0.001), and overall survival (OS) (HR: 0.82; 95% CI: 0.72-0.95; = 0.006). : While the neo-RAS-WT window is transient in non-shedding, it is durable in neo-RAS-WT patients, persisting until disease progression. These findings highlight the potential utility of ctDNA testing in refining treatment strategies for RAS-mutant mCR.
在转移性结直肠癌(mCRC)中,液体活检能够识别出“新RAS野生型(WT)”,这是一个以RAS突变消失为特征的短暂阶段,对重新敏感于EGFR阻断具有重要的临床意义。本研究旨在前瞻性地追踪接受一线及后续全身治疗的RAS突变型mCRC患者循环肿瘤DNA(ctDNA)中“新RAS野生型”的动态变化。
共分析了35例患者的380份连续血样。每位患者在一线及后续治疗期间每隔三个月提供中位数为10份的ctDNA样本。患者被分为三组:新RAS野生型、非脱落型和持续突变型。
在一线治疗期间,68%的患者转变为RAS野生型。其中,17%为新RAS野生型,而大多数被归类为非脱落型。在二线治疗中,新RAS野生型的比例增加到34%,在三线治疗期间降至8.5%。与非脱落型患者相比,新RAS野生型患者的新RAS野生型窗口持续时间显著更长(P = 0.037)。与持续突变型患者相比,达到RAS野生型状态的患者无进展生存期(PFS)有所改善,在所有治疗线中均观察到显著差异:一线(P = 0.004)、二线(P < 0.0001)和三线(P = 0.001)。多变量分析显示,RAS野生型窗口的持续时间与延长的一线PFS(HR:0.78;95%CI:0.69 - 0.89;P < 0.0001)、二线PFS(HR:0.66;95%CI:0.52 - 0.84;P = 0.001)和总生存期(OS)(HR:0.82;95%CI:0.72 - 0.95;P = 0.006)相关。
虽然新RAS野生型窗口在非脱落型中是短暂的,但在新RAS野生型患者中是持久的,一直持续到疾病进展。这些发现突出了ctDNA检测在优化RAS突变型mCRC治疗策略方面的潜在效用。
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