Chromatin extrusion explains key features of loop and domain formation in wild-type and engineered genomes
ORAL
Abstract
Our recent kilobase-resolution genome-wide maps of DNA self-contacts demonstrated that mammalian genomes are organized into domains and loops demarcated by the DNA-binding protein CTCF. Here, we combine these maps with new Hi-C, microscopy, and genome-editing experiments to study the physical structure of chromatin fibers, domains, and loops. We find that domains are inconsistent with equilibrium and fractal models. Instead, we use physical simulations to study two models of genome folding. In one, intermonomer attraction during condensation leads to formation of an anisotropic ``tension globule.'' In the other, CTCF and cohesin act together to extrude unknotted loops. Both models are consistent with the observed domains and loops. However, the extrusion model explains a far wider array of observations, such as why the CTCF-binding motifs at pairs of loop anchors lie in the convergent orientation. Finally, we perform 13 genome-editing experiments examining the effect of altering CTCF-binding sites on chromatin folding. The extrusion model predicts \textit{in silico} the experimental maps using only CTCF-binding sites. Thus, we show that it is possible to disrupt, restore, and move loops and domains using targeted mutations as small as a single base pair.
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Authors
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Adrian Sanborn
Stanford
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Suhas Rao
Stanford
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Su-Chen Huang
Baylor College of Medicine
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Neva Durand
Baylor College of Medicine
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Miriam Huntley
Baylor College of Medicine
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Andrew Jewett
Baylor College of Medicine
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Ivan Bochkov
Baylor College of Medicine
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Dharmaraj Chinnappan
Baylor College of Medicine
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Ashok Cutkosky
Baylor College of Medicine
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Jian Li
Baylor College of Medicine
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Kristopher Geeting
Baylor College of Medicine
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Doug McKenna
Baylor College of Medicine
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Elena Stamenova
Baylor College of Medicine
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Andreas Gnirke
Broad Institute
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Alexandre Melnikov
Broad Institute
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Eric Lander
Broad Institute
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Erez Aiden
Baylor College of Medicine