Cis-Acting Factors Causing Secondary Epimutations: Impact on the Risk for Cancer and Other Diseases.
Miguel Ruiz de la CruzAldo De la Cruz MontoyaErnesto Arturo Rojas-JiménezHéctor Martínez GregorioClara Estela Díaz VelásquezJimena Paredes de la VegaFidel de la Cruz Hernández-HernándezFelipe Vaca PaniaguaPublished in: Cancers (2021)
Epigenetics affects gene expression and contributes to disease development by alterations known as epimutations. Hypermethylation that results in transcriptional silencing of tumor suppressor genes has been described in patients with hereditary cancers and without pathogenic variants in the coding region of cancer susceptibility genes. Although somatic promoter hypermethylation of these genes can occur in later stages of the carcinogenic process, constitutional methylation can be a crucial event during the first steps of tumorigenesis, accelerating tumor development. Primary epimutations originate independently of changes in the DNA sequence, while secondary epimutations are a consequence of a mutation in a cis or trans-acting factor. Secondary epimutations have a genetic basis in cis of the promoter regions of genes involved in familial cancers. This highlights epimutations as a novel carcinogenic mechanism whose contribution to human diseases is underestimated by the scarcity of the variants described. In this review, we provide an overview of secondary epimutations and present evidence of their impact on cancer. We propose the necessity for genetic screening of loci associated with secondary epimutations in familial cancer as part of prevention programs to improve molecular diagnosis, secondary prevention, and reduce the mortality of these diseases.
Keyphrases
- genome wide
- gene expression
- papillary thyroid
- dna methylation
- copy number
- squamous cell
- transcription factor
- lymph node metastasis
- endothelial cells
- childhood cancer
- public health
- cardiovascular disease
- early onset
- type diabetes
- coronary artery disease
- single molecule
- genome wide identification
- young adults
- amino acid
- bioinformatics analysis
- cell free
- genome wide analysis
- circulating tumor cells