AI Article Synopsis

  • Identified split 8-mers in proximal promoters consist of two 4-mer transcription factor binding sites (TFBS) separated by 1 to 30 base pairs, allowing for precise localization.
  • The study reveals that overlapping ETS⇔ETS and ETS⇔CRE motifs can be bound simultaneously by specific proteins without conflict, while certain factors like ETV5 and CREB inhibit each other's binding to these motifs.
  • The ETS⇔CRE motif is prevalent in the human genome, particularly in regulatory regions, and is associated with genes that regulate mRNA processing, cellular functions, and stress responses, indicating its importance in gene regulation.

Article Abstract

Previously, we identified 8-bps long DNA sequences (8-mers) that localize in human proximal promoters and grouped them into known transcription factor binding sites (TFBS). We now examine split 8-mers consisting of two 4-mers separated by 1-bp to 30-bps (X(4)-N(1-30)-X(4)) to identify pairs of TFBS that localize in proximal promoters at a precise distance. These include two overlapping TFBS: the ETS⇔ETS motif ((C/G)CCGGAAGCGGAA) and the ETS⇔CRE motif ((C/G)CGGAAGTGACGTCAC). The nucleotides in bold are part of both TFBS. Molecular modeling shows that the ETS⇔CRE motif can be bound simultaneously by both the ETS and the B-ZIP domains without protein-protein clashes. The electrophoretic mobility shift assay (EMSA) shows that the ETS protein GABPα and the B-ZIP protein CREB preferentially bind to the ETS⇔CRE motif only when the two TFBS overlap precisely. In contrast, the ETS domain of ETV5 and CREB interfere with each other for binding the ETS⇔CRE. The 11-mer (CGGAAGTGACG), the conserved part of the ETS⇔CRE motif, occurs 226 times in the human genome and 83% are in known regulatory regions. In vivo GABPα and CREB ChIP-seq peaks identified the ETS⇔CRE as the most enriched motif occurring in promoters of genes involved in mRNA processing, cellular catabolic processes, and stress response, suggesting that a specific class of genes is regulated by this composite motif.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3464117PMC
http://dx.doi.org/10.1534/g3.112.004002DOI Listing

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