RNA Editing in Cancer Progression

SIMPLE SUMMARY: Recent evidence from whole-exome and whole-genome sequencing approaches revealed a complex genomic landscape for many cancers. In addition to somatic mutations and alternative splicing changes, genetic information can also be altered by RNA editing, which enables alterations of genome information in a very dynamic and flexible way. Influenced by both external factors and microenvironmental signals, RNA editing deeply contributes to cancer morphological plasticity. ABSTRACT: Coding and noncoding RNA molecules play their roles in ensuring cell function and tissue homeostasis in an ordered and systematic fashion. RNA chemical modifications can occur both at bases and ribose sugar, and, similarly to DNA and histone modifications, can be written, erased, and recognized by the corresponding enzymes, thus modulating RNA activities and fine-tuning gene expression programs. RNA editing is one of the most prevalent and abundant forms of post-transcriptional RNA modification in normal physiological processes. By altering the sequences of mRNAs, it makes them different from the corresponding genomic template. Hence, edited mRNAs can produce protein isoforms that are functionally different from the corresponding genome-encoded variants. Abnormalities in regulatory enzymes and changes in RNA-modification patterns are closely associated with the occurrence and development of various human diseases, including cancer. To date, the roles played by RNA modifications in cancer are gathering increasing interest. In this review, we focus on the role of RNA editing in cancer transformation and provide a new perspective on its impact on tumorigenesis, by regulating cell proliferation, differentiation, invasion, migration, stemness, metabolism, and drug resistance.