The amniote-conserved DNA-binding domain of CGGBP1 restricts cytosine methylation of transcription factor binding sites in proximal promoters to regulate gene expression

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dc.contributor.author Morbia, Ishani
dc.contributor.author Kumar, Praveen
dc.contributor.author Satish, Aditi Lakshmi
dc.contributor.author Mudgal, Akanksha
dc.contributor.author Datta, Subhamoy
dc.contributor.author Singh, Umashankar
dc.coverage.spatial United Kingdom
dc.date.accessioned 2024-11-28T09:51:31Z
dc.date.available 2024-11-28T09:51:31Z
dc.date.issued 2024-12
dc.identifier.citation Morbia, Ishani; Kumar, Praveen; Satish, Aditi Lakshmi; Mudgal, Akanksha; Datta, Subhamoy and Singh, Umashankar, "The amniote-conserved DNA-binding domain of CGGBP1 restricts cytosine methylation of transcription factor binding sites in proximal promoters to regulate gene expression", BMC Genomic Data, DOI: 10.1186/s12863-024-01282-2, vol. 25, no. 01, Dec. 2024.
dc.identifier.issn 2730-6844
dc.identifier.uri https://doi.org/10.1186/s12863-024-01282-2
dc.identifier.uri https://repository.iitgn.ac.in/handle/123456789/10795
dc.description.abstract CGGBP1 is a GC-rich DNA-binding protein which is important for genomic integrity, gene expression and epigenome maintenance through regulation of CTCF occupancy and cytosine methylation. It has remained unclear how CGGBP1 integrates multiple diverse functions with its simple architecture of only a DNA-binding domain tethered to a C-terminal tail with low structural rigidity. We have used truncated forms of CGGBP1 with or without the DNA-binding domain (DBD) to assay cytosine methylation and global gene expression. Proximal promoters of CGGBP1-repressed genes, although significantly GC-poor, contain GC-rich transcription factor binding motifs and exhibit base compositions indicative of low C-T transition rates due to prevention of cytosine methylation. Genome-wide analyses of cytosine methylation and binding of CGGBP1 DBD show that CGGBP1 restricts cytosine methylation in a manner that depends on its DBD and its DNA-binding. The CGGBP1-repressed genes show an increase in promoter cytosine methylation alongside a decrease in transcript abundance when the DBD-deficient CGGBP1 is expressed. Our findings suggest that CGGBP1 protects transcription factor binding sites (TFBS) from cytosine methylation-associated loss and thereby regulates gene expression. By analysing orthologous promoter sequences we show that restriction of cytosine methylation is a function of CGGBP1 progressively acquired during vertebrate evolution. A superimposition of our results and evolution of CGGBP1 suggests that mitigation of cytosine methylation is majorly achieved by its N-terminal DBD. Our results position CGGBP1 DNA-binding as a major evolutionarily acquired mechanism through which it keeps cytosine methylation under check and regulates TFBS retention and gene activity.
dc.description.statementofresponsibility by Ishani Morbia, Praveen Kumar, Aditi Lakshmi Satish, Akanksha Mudgal, Subhamoy Datta and Umashankar Singh
dc.format.extent vol. 25, no. 01
dc.language.iso en_US
dc.publisher BioMed Central
dc.subject CGGBP1
dc.subject TFBS
dc.subject DNA sequence motifs
dc.subject Evolution
dc.title The amniote-conserved DNA-binding domain of CGGBP1 restricts cytosine methylation of transcription factor binding sites in proximal promoters to regulate gene expression
dc.type Article
dc.relation.journal BMC Genomic Data


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