4.3 Article

Changes in DNA methylation hallmark alterations in chromatin accessibility and gene expression for eye lens differentiation

期刊

EPIGENETICS & CHROMATIN
卷 15, 期 1, 页码 -

出版社

BMC
DOI: 10.1186/s13072-022-00440-z

关键词

DNA methylation; Bisulfite sequencing; RNA-seq; ATAC-seq; Lens; Differentiation; Gene regulation; Chromatin; Transcriptional regulation

资金

  1. National Institutes of Health, USA
  2. National Eye Institute, USA [EY029708]

向作者/读者索取更多资源

This study explores the relationships between mCG methylation, chromatin accessibility, and gene expression during the differentiation of eye lens epithelial cells into fiber cells. The results show that changes in mCG levels are inversely correlated with the expression of genes associated with lens fiber cells or lens epithelial cells. The study also suggests a role for DNA methylation in the regulation of transcription factors important for lens cell differentiation.
Background Methylation at cytosines (mCG) is a well-known regulator of gene expression, but its requirements for cellular differentiation have yet to be fully elucidated. A well-studied cellular differentiation model system is the eye lens, consisting of a single anterior layer of epithelial cells that migrate laterally and differentiate into a core of fiber cells. Here, we explore the genome-wide relationships between mCG methylation, chromatin accessibility and gene expression during differentiation of eye lens epithelial cells into fiber cells. Results Whole genome bisulfite sequencing identified 7621 genomic loci exhibiting significant differences in mCG levels between lens epithelial and fiber cells. Changes in mCG levels were inversely correlated with the differentiation state-specific expression of 1285 genes preferentially expressed in either lens fiber or lens epithelial cells (Pearson correlation r = - 0.37, p < 1 x 10(-42)). mCG levels were inversely correlated with chromatin accessibility determined by assay for transposase-accessible sequencing (ATAC-seq) (Pearson correlation r = - 0.86, p < 1 x 10(-300)). Many of the genes exhibiting altered regions of DNA methylation, chromatin accessibility and gene expression levels in fiber cells relative to epithelial cells are associated with lens fiber cell structure, homeostasis and transparency. These include lens crystallins (CRYBA4, CRYBB1, CRYGN, CRYBB2), lens beaded filament proteins (BFSP1, BFSP2), transcription factors (HSF4, SOX2, HIF1A), and Notch signaling pathway members (NOTCH1, NOTCH2, HEY1, HES5). Analysis of regions exhibiting cell-type specific alterations in DNA methylation revealed an overrepresentation of consensus sequences of multiple transcription factors known to play key roles in lens cell differentiation including HIF1A, SOX2, and the MAF family of transcription factors. Conclusions Collectively, these results link DNA methylation with control of chromatin accessibility and gene expression changes required for eye lens differentiation. The results also point to a role for DNA methylation in the regulation of transcription factors previously identified to be important for lens cell differentiation.

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