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      Topologically Associating Domains: An invariant framework or a dynamic scaffold?

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          Abstract

          Metazoan genomes are organized into regions of topologically associating domains (TADs). TADs are demarcated by border elements, which are enriched for active genes and high occupancy architectural protein binding sites. We recently demonstrated that 3D chromatin architecture is dynamic in response to heat shock, a physiological stress that downregulates transcription and causes a global redistribution of architectural proteins. We utilized a quantitative measure of border strength after heat shock, transcriptional inhibition, and architectural protein knockdown to demonstrate that changes in both transcription and architectural protein occupancy contribute to heat shock-induced TAD dynamics. Notably, architectural proteins appear to play a more important role in altering 3D chromatin architecture. Here, we discuss the implications of our findings on previous studies evaluating the dynamics of TAD structure during cellular differentiation. We propose that the subset of variable TADs observed after differentiation are representative of cell-type specific gene expression and are biologically significant.

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          Author and article information

          Journal
          Nucleus
          Nucleus (Austin, Tex.)
          Informa UK Limited
          1949-1042
          1949-1034
          2015
          : 6
          : 6
          Affiliations
          [1 ] a Department of Biology ; Emory University ; Atlanta , GA USA.
          Article
          10.1080/19491034.2015.1096467
          4915497
          26418477
          90349185-3471-4c6c-8a5d-f5a9d3915a62
          History

          3D architecture,CTCF,TAD,architectural proteins,chromatin,differentiation,epigenetics,heat shock,insulators

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