Clinical and Functional Characterization of AtypicalKRAS/NRASMutations in Metastatic Colorectal Cancer

克拉斯 神经母细胞瘤RAS病毒癌基因同源物 结直肠癌 癌症研究 突变 医学 生物 外显子 癌症 肿瘤科 遗传学 赫拉 基因
作者
Jonathan M. Loree,Yucai Wang,Muddassir Syed,Alexey V. Sorokin,Oluwadara Coker,Joanne Xiu,Benjamin A. Weinberg,Ari M. Vanderwalde,Anteneh Tesfaye,Victoria M. Raymond,Benjamin Miron,Gabi Tarcic,Ori Zelichov,Russell R. Broaddus,Patrick Kwok Shing Ng,Kang Jin Jeong,Yiu Huen Tsang,Gordon B. Mills,Michael J. Overman,Axel Grothey
出处
期刊:Clinical Cancer Research [American Association for Cancer Research]
卷期号:27 (16): 4587-4598 被引量:36
标识
DOI:10.1158/1078-0432.ccr-21-0180
摘要

Abstract Purpose: Mutations in KRAS/NRAS (RAS) predict lack of anti-EGFR efficacy in metastatic colorectal cancer (mCRC). However, it is unclear if all RAS mutations have similar impact, and atypical mutations beyond those in standard guidelines exist. Experimental Design: We reviewed 7 tissue and 1 cell-free DNA cohorts of 9,485 patients to characterize atypical RAS variants. Using an in vitro cell-based assay (functional annotation for cancer treatment), Ba/F3 transformation, and in vivo xenograft models of transduced isogenic clones, we assessed signaling changes across mutations. Results: KRAS exon 2, extended RAS, and atypical RAS mutations were noted in 37.8%, 9.5%, and 1.2% of patients, respectively. Among atypical variants, KRAS L19F, Q22K, and D33E occurred at prevalence ≥0.1%, whereas no NRAS codon 117/146 and only one NRAS codon 59 mutation was noted. Atypical RAS mutations had worse overall survival than RAS/BRAF wild-type mCRC (HR, 2.90; 95% confidence interval, 1.24–6.80; P = 0.014). We functionally characterized 114 variants with the FACT assay. All KRAS exon 2 and extended RAS mutations appeared activating. Of 57 atypical RAS variants characterized, 18 (31.6%) had signaling below wild-type, 23 (40.4%) had signaling between wild-type and activating control, and 16 (28.1%) were hyperactive beyond the activating control. Ba/F3 transformation (17/18 variants) and xenograft model (7/8 variants) validation was highly concordant with FACT results, and activating atypical variants were those that occurred at highest prevalence in clinical cohorts. Conclusions: We provide best available evidence to guide treatment when atypical RAS variants are identified. KRAS L19F, Q22K, D33E, and T50I are more prevalent than many guideline-included RAS variants and functionally relevant.
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