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  • Analysis of Genetically Diverse Macrophages Reveals Local and Domain-wide Mechanisms that Control Transcription Factor Binding and Function.

Analysis of Genetically Diverse Macrophages Reveals Local and Domain-wide Mechanisms that Control Transcription Factor Binding and Function.

Cell (2018-05-22)
Verena M Link, Sascha H Duttke, Hyun B Chun, Inge R Holtman, Emma Westin, Marten A Hoeksema, Yohei Abe, Dylan Skola, Casey E Romanoski, Jenhan Tao, Gregory J Fonseca, Ty D Troutman, Nathanael J Spann, Tobias Strid, Mashito Sakai, Miao Yu, Rong Hu, Rongxin Fang, Dirk Metzler, Bing Ren, Christopher K Glass
摘要

Non-coding genetic variation is a major driver of phenotypic diversity and allows the investigation of mechanisms that control gene expression. Here, we systematically investigated the effects of >50 million variations from five strains of mice on mRNA, nascent transcription, transcription start sites, and transcription factor binding in resting and activated macrophages. We observed substantial differences associated with distinct molecular pathways. Evaluating genetic variation provided evidence for roles of ∼100 TFs in shaping lineage-determining factor binding. Unexpectedly, a substantial fraction of strain-specific factor binding could not be explained by local mutations. Integration of genomic features with chromatin interaction data provided evidence for hundreds of connected cis-regulatory domains associated with differences in transcription factor binding and gene expression. This system and the >250 datasets establish a substantial new resource for investigation of how genetic variation affects cellular phenotypes.

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Sigma-Aldrich
双琥珀酰亚胺戊二酸酯, ≥97.0% (CHN)
Sigma-Aldrich
抗二甲基组蛋白H3(Lys4)抗体, Upstate®, from rabbit
Sigma-Aldrich
抗三甲基组蛋白H3(Lys4)抗体,克隆MC315,兔单克隆, culture supernatant, clone MC315, Upstate®