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Interplay of cis and trans mechanisms driving transcription factor binding and gene expression evolution

Authors :
Anastasiya Kazachenka
Bianca M. Schmitt
Duncan T. Odom
John C. Marioni
David Thybert
Aisling M. Redmond
Tim F. Rayner
Anne C. Ferguson-Smith
Emily S. W. Wong
Frances Connor
Christine Feig
Paul Flicek
Feig, Christine [0000-0003-1385-7049]
Ferguson-Smith, Anne [0000-0003-4996-9990]
Marioni, John [0000-0001-9092-0852]
Odom, Duncan [0000-0001-6201-5599]
Apollo - University of Cambridge Repository
Source :
Nature Communications, Vol 8, Iss 1, Pp 1-13 (2017), Nature Communications
Publication Year :
2016
Publisher :
Cold Spring Harbor Laboratory, 2016.

Abstract

Noncoding regulatory variants play a central role in the genetics of human diseases and in evolution. Here we measure allele-specific transcription factor binding occupancy of three liver-specific transcription factors between crosses of two inbred mouse strains to elucidate the regulatory mechanisms underlying transcription factor binding variations in mammals. Our results highlight the pre-eminence of cis-acting variants on transcription factor occupancy divergence. Transcription factor binding differences linked to cis-acting variants generally exhibit additive inheritance, while those linked to trans-acting variants are most often dominantly inherited. Cis-acting variants lead to local coordination of transcription factor occupancies that decay with distance; distal coordination is also observed and may be modulated by long-range chromatin contacts. Our results reveal the regulatory mechanisms that interplay to drive transcription factor occupancy, chromatin state, and gene expression in complex mammalian cell states.<br />“Variation in the noncoding regulatory sequences in the genome plays important roles in human disease and evolution. Here, the authors use F1 mouse hybrids to shed light on the regulatory mechanisms mediating transcription factor binding, chromatin state and gene expression in mammalian cells.”

Details

Language :
English
Database :
OpenAIRE
Journal :
Nature Communications, Vol 8, Iss 1, Pp 1-13 (2017), Nature Communications
Accession number :
edsair.doi.dedup.....07b497643cd9fdd3d34172e1aab9c510
Full Text :
https://doi.org/10.1101/059873