mutations in colorectal cancer have been studied over the past several decades. V600E mutation, a class I mutation, is the most common oncogenic alteration in colorectal cancer. Until recently, the V600E mutation was not among actionable genes for colorectal cancer. However, recent discoveries have revealed therapeutic opportunities. The with or without MEK inhibition combined with epidermal growth factor receptor-directed therapy was recently found to be an effective therapy choice for patients with advanced-stage V600-mutant colorectal cancer. However, it is essential to distinguish patients with V600E-mutant mismatch repair-deficient colorectal cancer from those with mismatch repair-proficient colorectal cancer, as immune checkpoint inhibitor therapy is more appealing in this subset of patients with colorectal cancer. This review article discusses the molecular characteristics of class I, II, and III mutants and their impact on the clinical behavior of colorectal cancer. We also review the recent progress in the targetability of mutations in colorectal cancer, which has led to changes in clinical practice and elaborates on innovative therapeutic approaches to enhance the efficacy of -targeting therapies, to achieve more durable responses.

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http://dx.doi.org/10.1200/OP.21.00160DOI Listing

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