RNA sequencing-based screen for reactivation of silenced alleles of autosomal genes.
Saumya GuptaDenis L LafontaineSebastien VigneauAsia MendelevichSvetlana VinogradovaKyomi J IgarashiAndrew BortvinClara F Alves-PereiraAnwesha NagAlexander A GimelbrantPublished in: G3 (Bethesda, Md.) (2022)
In mammalian cells, maternal and paternal alleles usually have similar transcriptional activity. Epigenetic mechanisms such as X-chromosome inactivation (XCI) and imprinting were historically viewed as rare exceptions to this rule. Discovery of autosomal monoallelic autosomal expression (MAE) a decade ago revealed an additional allele-specific mode regulating thousands of mammalian genes. Despite MAE prevalence, its mechanistic basis remains unknown. Using an RNA sequencing-based screen for reactivation of silenced alleles, we identified DNA methylation as key mechanism of MAE mitotic maintenance. In contrast with the all-or-nothing allelic choice in XCI, allele-specific expression in MAE loci is tunable, with exact allelic imbalance dependent on the extent of DNA methylation. In a subset of MAE genes, allelic imbalance was insensitive to DNA demethylation, implicating additional mechanisms in MAE maintenance in these loci. Our findings identify a key mechanism of MAE maintenance and provide basis for understanding the biological role of MAE.
Keyphrases
- genome wide
- dna methylation
- gene expression
- single cell
- poor prognosis
- copy number
- high throughput
- magnetic resonance
- small molecule
- computed tomography
- bioinformatics analysis
- risk factors
- pregnant women
- magnetic resonance imaging
- transcription factor
- body mass index
- cell cycle
- genome wide association study
- genome wide analysis