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'Stripe' transcription factors provide accessibility to co-binding partners in mammalian genomes

Authors :
Yongbing Zhao
Supriya V. Vartak
Andrea Conte
Xiang Wang
David A. Garcia
Evan Stevens
Seol Kyoung Jung
Kyong-Rim Kieffer-Kwon
Laura Vian
Timothy Stodola
Francisco Moris
Laura Chopp
Silvia Preite
Pamela L. Schwartzberg
Joseph M. Kulinski
Ana Olivera
Christelle Harly
Avinash Bhandoola
Elisabeth F. Heuston
David M. Bodine
Raul Urrutia
Arpita Upadhyaya
Matthew T. Weirauch
Gordon Hager
Rafael Casellas
Zhao, Y.
Vartak, S. V.
Conte, A.
Wang, X.
Garcia, D. A.
Stevens, E.
Kyoung Jung, S.
Kieffer-Kwon, K. -R.
Vian, L.
Stodola, T.
Moris, F.
Chopp, L.
Preite, S.
Schwartzberg, P. L.
Kulinski, J. M.
Olivera, A.
Harly, C.
Bhandoola, A.
Heuston, E. F.
Bodine, D. M.
Urrutia, R.
Upadhyaya, A.
Weirauch, M. T.
Hager, G.
Casellas, R.
Source :
Molecular cell. 82(18)
Publication Year :
2021

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.

Details

ISSN :
10974164
Volume :
82
Issue :
18
Database :
OpenAIRE
Journal :
Molecular cell
Accession number :
edsair.doi.dedup.....b3aa7283a073e3f8e1086eef862cab3f