AI Article Synopsis
- * The text reviews how these mutations overlap or occur uniquely in different CRC cases, examining the biological roles of KRAS and BRAF in cancer development and their different signaling pathways.
- * It also covers current treatment strategies targeting the RAS-RAF signaling pathways in metastatic CRC, while discussing the potential directions for future therapies.
Article Abstract
Colorectal cancer (CRC) is characterized by recurrent mutations deregulating key cell signaling cascades and providing the cancer cells with novel functional traits. Among the most frequent mutations in CRC are gain-of-function missense mutations in KRAS and BRAF. Oncogenic activation of KRAS and BRAF is mutually exclusive and occurs in approximately 40% and 10% of all CRCs, respectively. Here we summarize genetic alterations currently described in the literature and databases, indicating overlapping but also specific co-occurrences with either mutated BRAF or KRAS. We describe common and potentially specific biological functions of KRAS and BRAF oncoproteins in the intestinal epithelial cells and during initiation and progression of CRC. We discuss signal transduction networks, highlighting individual functions of oncogenic KRAS and BRAF in terms of feedback loops and their impact on treatment outcome. Finally, we give an update on current strategies of targeted therapeutic intervention in oncogenic RAS-RAF signaling networks for the treatment of metastatic CRC and outline future directions.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4673229 | PMC |
| http://dx.doi.org/10.18632/oncotarget.4750 | DOI Listing |
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