Summary
Colorectal cancer (CRC) is one of the most deadly and commonly diagnosed tumors worldwide. Several genes are involved in its development and progression. The most frequent mutations concern APC, KRAS, SMAD4, and TP53 genes, suggesting that CRC relies on the alteration of different pathways. However, with classic molecular approaches, it is not easy to simultaneously analyze the interconnections between these pathways. For this reason, we propose a computational model based on a huge chemical reaction network to simulate the effects induced on the global signaling associated with CRC by single or multiple concurrent mutations or by drug treatment. This approach displays several advantages. The model can quantify the alteration in the concentration of the proteins connected with the examined mutation. Moreover, working on the global signaling of CRC, it is possible to disclose unexpected interactions between the involved pathways, representing new therapeutic targets.
Highlights
Colorectal cancer relates to defects in many different pathways within cell signaling
Cell signaling is modeled as a chemical ration network with 10 interacting pathways
Global effects induced by single or multiple concurrent mutations are quantified
A possible extension of the model to account for a targeted drug is discussed
Competing Interest Statement
The authors have declared no competing interest.