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Translation initiation and its relevance in colorectal cancer.

Emma Minnee ,
William James Faller

Abstract

Protein synthesis is one of the most essential processes in every kingdom of life, and its dysregulation is a known driving force in cancer development. Multiple signaling pathways converge on the translation initiation machinery, and this plays a crucial role in regulating differential gene expression. In colorectal cancer, dysregulation of initiation results in translational reprogramming, which promotes the selective translation of mRNAs required for many oncogenic processes. The majority of upstream mutations found in colorectal cancer, including alterations in the WNT, MAPK, and PI3K\AKT pathways, have been demonstrated to play a significant role in translational reprogramming. Many translation initiation factors are also known to be dysregulated, resulting in translational reprogramming during tumor initiation and/or maintenance. In this review, we outline the role of translational reprogramming that occurs during colorectal cancer development and progression and highlight some of the most critical factors affecting the etiology of this disease.

More about this publication

The FEBS journal

Volume 288
Issue nr. 23
Pages 6635-6651
Publication date 01-12-2021

Full text links

Publisher website (DOI) 10.1111/febs.15690
Europe PubMed Central 33382175
Pubmed 33382175

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