Author: Liang, Jie; Perez-Rathke, Alan
Title: Minimalistic 3D Chromatin Models: Sparse Interactions in Single Cells Drive the Chromatin Fold and Form Many-Body Units Cord-id: ucltwtgw Document date: 2021_8_8
ID: ucltwtgw
Snippet: Computational modeling of 3D chromatin plays an important role in understanding the principles of genome organization. We discuss methods for modeling 3D chromatin structures, with focus on a minimalistic polymer model which inverts population Hi-C into high-resolution, high-coverage single-cell chromatin conformations. Utilizing only basic physical properties such as nuclear volume and no adjustable parameters, this model uncovers a few specific Hi-C interactions (15-35 for enhancerrich loci in
Document: Computational modeling of 3D chromatin plays an important role in understanding the principles of genome organization. We discuss methods for modeling 3D chromatin structures, with focus on a minimalistic polymer model which inverts population Hi-C into high-resolution, high-coverage single-cell chromatin conformations. Utilizing only basic physical properties such as nuclear volume and no adjustable parameters, this model uncovers a few specific Hi-C interactions (15-35 for enhancerrich loci in human cells) that can fold chromatin into individual conformations consistent with single-cell imaging, Dip-C, and FISH-measured genomic distance distributions. Aggregating an ensemble of conformations also reproduces population Hi-C interaction frequencies. Furthermore, this single-cell modeling approach allows quantification of structural heterogeneity and discovery of specific many-body units of chromatin interactions. This minimalistic 3D chromatin polymer model has revealed a number of insights: 1) chromatin scaling rules are a result of volume-confined polymers; 2) TADs form as a byproduct of 3D chromatin folding driven by specific interactions; 3) chromatin folding at many loci is driven by a small number of specific interactions; 4) cell subpopulations equipped with different chromatin structural scaffolds are developmental stage-dependent; and 5) characterization of the functional landscape and epigenetic marks of many-body units which are simultaneously spatially co-interacting within enhancer-rich, euchromatic regions. The implications of these findings in understanding the genome structure-function relationship are also discussed.
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