| Literature DB >> 35863348 |
Yongbing Zhao1, Supriya V Vartak2, Andrea Conte2, Xiang Wang2, David A Garcia3, Evan Stevens4, Seol Kyoung Jung2, Kyong-Rim Kieffer-Kwon4, Laura Vian4, Timothy Stodola5, Francisco Moris6, Laura Chopp7, Silvia Preite8, Pamela L Schwartzberg8, Joseph M Kulinski9, Ana Olivera9, Christelle Harly10, Avinash Bhandoola10, Elisabeth F Heuston11, David M Bodine11, Raul Urrutia5, Arpita Upadhyaya12, Matthew T Weirauch13, Gordon Hager14, Rafael Casellas15.
Abstract
Regulatory elements activate promoters by recruiting transcription factors (TFs) to specific motifs. Notably, TF-DNA interactions often depend on cooperativity with colocalized partners, suggesting an underlying cis-regulatory syntax. To explore TF cooperativity in mammals, we analyze ∼500 mouse and human primary cells by combining an atlas of TF motifs, footprints, ChIP-seq, transcriptomes, and accessibility. We uncover two TF groups that colocalize with most expressed factors, forming stripes in hierarchical clustering maps. The first group includes lineage-determining factors that occupy DNA elements broadly, consistent with their key role in tissue-specific transcription. The second one, dubbed universal stripe factors (USFs), comprises ∼30 SP, KLF, EGR, and ZBTB family members that recognize overlapping GC-rich sequences in all tissues analyzed. Knockouts and single-molecule tracking reveal that USFs impart accessibility to colocalized partners and increase their residence time. Mammalian cells have thus evolved a TF superfamily with overlapping DNA binding that facilitate chromatin accessibility.Entities:
Keywords: DNA motifs; chromatin accessibility; enhancer syntax; gene expression; mammalian genomes; regulatory elements; single molecule tracking; transcription factors
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Year: 2022 PMID: 35863348 PMCID: PMC9481673 DOI: 10.1016/j.molcel.2022.06.029
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 19.328