KRASG12D突变的转移性结直肠癌:一种新出现的靶向变异的临床、分子、免疫学和预后特征

IF 5.3 2区 医学 Q1 ONCOLOGY
JCO precision oncology Pub Date : 2024-11-01 Epub Date: 2024-11-07 DOI:10.1200/PO.24.00329
Roberto Moretto, Daniele Rossini, Sabina Murgioni, Paolo Ciracì, Vincenzo Nasca, Marco Maria Germani, Maria Alessandra Calegari, Guglielmo Vetere, Rossana Intini, Ada Taravella, Vittorio Studiale, Chiara Boccaccio, Alessandro Passardi, Emiliano Tamburini, Alberto Zaniboni, Lisa Salvatore, Filippo Pietrantonio, Sara Lonardi, Gianluca Masi, Chiara Cremolini
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引用次数: 0

摘要

目的:约 10%-12%的转移性结直肠癌(mCRC)存在 KRASG12D 突变(mut)。最近,新型 KRASG12D 抑制剂已经开发出来,目前正在进行包括 mCRC 在内的实体瘤 I/II 期临床试验。我们的目的是对 KRASG12D 突变的 mCRC 的临床、分子、免疫学和预后特征进行全面分析,为未来试验的设计和解释提供依据:我们对比较5-氟尿嘧啶、亮菌素、奥沙利铂和伊立替康(FOLFOXIRI)/贝伐单抗(bev)与双联疗法(5-氟尿嘧啶、亮菌素和奥沙利铂或5-氟尿嘧啶、亮菌素和伊立替康)/贝伐单抗的III期TRIBE和TRIBE2研究进行了汇总分析:在854例有KRASG12D突变状态的患者中,136例(16%)为KRASG12D突变。KRASG12D突变患者多为右侧原发肿瘤,与其他RAS突变和全野生型(wt)患者相比,出现肝转移的可能性较小。与BRAFV600E突变组相比,KRASG12D突变组患者的原发肿瘤多为左侧,诊断时原发肿瘤已切除,且东部合作肿瘤学组(Eastern Cooperative Oncology Group)的预后状态为0。总体而言,KRASG12D突变患者与其他RAS突变患者的预后差异并不明显,其他特定的KRAS或NRAS热点突变也是如此。在KRASG12D突变与FOLFOXIRI/bev和doublets/bev的获益之间没有观察到相互作用效应。与其他RAS突变和所有wt相比,KRASG12D突变肿瘤中PIK3CA突变更常见:结论:对KRASG12D突变mCRC患者的特征和预期预后进行详细评估,可能有助于规划未来针对该亚组的研究。PI3K/PTEN/Akt通路激活改变的高发生率可能会影响靶向策略的疗效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
KRASG12D-Mutated Metastatic Colorectal Cancer: Clinical, Molecular, Immunologic, and Prognostic Features of a New Emerging Targeted Alteration.

Purpose: KRASG12D mutation (mut) occurs in about 10%-12% of metastatic colorectal cancer (mCRC). Recently, novel KRASG12D inhibitors have been developed and are currently under investigation in phase I/II clinical trials in solid tumors including mCRC. We aimed at performing a comprehensive characterization of clinical, molecular, immunologic, and prognostic features of KRASG12D-mutated mCRC to inform the design and the interpretation of future trials.

Methods: We performed a pooled analysis of phase III TRIBE and TRIBE2 studies comparing 5-fluorouracil, leucovorin, oxaliplatin, and irinotecan (FOLFOXIRI)/bevacizumab (bev) to doublets (5-fluorouracil, leucovorin, and oxaliplatin or 5-fluorouracil, leucovorin, and irinotecan)/bev.

Results: One hundred and thirty-six (16%) of 854 patients with available KRASG12D mutational status were KRASG12D mutated. KRASG12D-mutated patients had more frequently right-sided primary tumor and were less likely to present liver-only metastases with respect to other RAS mutated and all-wild-type (wt) patients. Compared with the BRAFV600E-mutated group, KRASG12D-mutated patients had more frequently left-sided primary tumor, resected primary tumor at the time of diagnosis, and Eastern Cooperative Oncology Group performance status 0. KRASG12D-mutated patients had better prognosis than BRAFV600E-mutated and worse prognosis than all wt patients. No prognostic difference was evident between KRASG12D mut and other RAS mut patients overall or according to other specific KRAS or NRAS hotspot mutations. No interaction effect was observed between KRASG12D mut and the benefit provided by FOLFOXIRI/bev compared with doublets/bev. PIK3CA mut were reported more frequently among KRASG12D-mutated tumors compared with both other RAS mut and all wt.

Conclusion: A detail estimation of KRASG12D mut mCRC patients' characteristics and expected outcomes may be useful when planning future studies in this subgroup. The high prevalence of PI3K/PTEN/Akt pathway activating alterations may affect the efficacy of targeted strategies.

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