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Single-molecule regulatory architectures captured by chromatin fiber sequencing.

Andrew Ben StergachisBrian M DeboEric HaugenL Stirling ChurchmanJohn A Stamatoyannopoulos
Published in: Science (New York, N.Y.) (2020)
Gene regulation is chiefly determined at the level of individual linear chromatin molecules, yet our current understanding of cis-regulatory architectures derives from fragmented sampling of large numbers of disparate molecules. We developed an approach for precisely stenciling the structure of individual chromatin fibers onto their composite DNA templates using nonspecific DNA N6-adenine methyltransferases. Single-molecule long-read sequencing of chromatin stencils enabled nucleotide-resolution readout of the primary architecture of multikilobase chromatin fibers (Fiber-seq). Fiber-seq exposed widespread plasticity in the linear organization of individual chromatin fibers and illuminated principles guiding regulatory DNA actuation, the coordinated actuation of neighboring regulatory elements, single-molecule nucleosome positioning, and single-molecule transcription factor occupancy. Our approach and results open new vistas on the primary architecture of gene regulation.
Keyphrases
  • single molecule
  • transcription factor
  • genome wide
  • dna damage
  • atomic force microscopy
  • living cells
  • gene expression
  • dna binding
  • single cell
  • genome wide identification
  • dna methylation
  • rna seq
  • high resolution
  • cell free