Ultrastructural Details of Mammalian Chromosome Architecture

Nils Krietenstein; Sameer Abraham; Sergey V Venev; Nezar Abdennur; Johan Gibcus; Tsung-Han S Hsieh; Krishna Mohan Parsi; Liyan Yang; René Maehr; Leonid A Mirny; Job Dekker; Oliver J Rando

doi:10.1016/j.molcel.2020.03.003

Ultrastructural Details of Mammalian Chromosome Architecture

Nils Krietenstein, Sameer Abraham, Sergey V Venev, Nezar Abdennur, Johan Gibcus, Tsung-Han S Hsieh, Krishna Mohan Parsi, Liyan Yang, René Maehr, Leonid A Mirny, Job Dekker, Oliver J Rando

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

337 Citationer (Scopus)

Abstract

Over the past decade, 3C-related methods have provided remarkable insights into chromosome folding in vivo. To overcome the limited resolution of prior studies, we extend a recently developed Hi-C variant, Micro-C, to map chromosome architecture at nucleosome resolution in human ESCs and fibroblasts. Micro-C robustly captures known features of chromosome folding including compartment organization, topologically associating domains, and interactions between CTCF binding sites. In addition, Micro-C provides a detailed map of nucleosome positions and localizes contact domain boundaries with nucleosomal precision. Compared to Hi-C, Micro-C exhibits an order of magnitude greater dynamic range, allowing the identification of ∼20,000 additional loops in each cell type. Many newly identified peaks are localized along extrusion stripes and form transitive grids, consistent with their anchors being pause sites impeding cohesin-dependent loop extrusion. Our analyses comprise the highest-resolution maps of chromosome folding in human cells to date, providing a valuable resource for studies of chromosome organization.

Originalsprog	Engelsk
Tidsskrift	Molecular Cell
Vol/bind	78
Udgave nummer	3
Sider (fra-til)	554-565.e7
ISSN	1097-2765
DOI	https://doi.org/10.1016/j.molcel.2020.03.003
Status	Udgivet - 7 maj 2020
Udgivet eksternt	Ja

Bibliografisk note

Adgang til dokumentet

10.1016/j.molcel.2020.03.003

Citationsformater

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title = "Ultrastructural Details of Mammalian Chromosome Architecture",

abstract = "Over the past decade, 3C-related methods have provided remarkable insights into chromosome folding in vivo. To overcome the limited resolution of prior studies, we extend a recently developed Hi-C variant, Micro-C, to map chromosome architecture at nucleosome resolution in human ESCs and fibroblasts. Micro-C robustly captures known features of chromosome folding including compartment organization, topologically associating domains, and interactions between CTCF binding sites. In addition, Micro-C provides a detailed map of nucleosome positions and localizes contact domain boundaries with nucleosomal precision. Compared to Hi-C, Micro-C exhibits an order of magnitude greater dynamic range, allowing the identification of ∼20,000 additional loops in each cell type. Many newly identified peaks are localized along extrusion stripes and form transitive grids, consistent with their anchors being pause sites impeding cohesin-dependent loop extrusion. Our analyses comprise the highest-resolution maps of chromosome folding in human cells to date, providing a valuable resource for studies of chromosome organization.",

keywords = "Animals, CCCTC-Binding Factor/metabolism, Cells, Cultured, Chromatin/chemistry, Chromosomes, Human/ultrastructure, Chromosomes, Mammalian/ultrastructure, Embryonic Stem Cells/cytology, Fibroblasts/cytology, Humans, Male, Mammals/genetics, Nucleosomes/metabolism, Signal-To-Noise Ratio",

author = "Nils Krietenstein and Sameer Abraham and Venev, {Sergey V} and Nezar Abdennur and Johan Gibcus and Hsieh, {Tsung-Han S} and Parsi, {Krishna Mohan} and Liyan Yang and Ren{\'e} Maehr and Mirny, {Leonid A} and Job Dekker and Rando, {Oliver J}",

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doi = "10.1016/j.molcel.2020.03.003",

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T1 - Ultrastructural Details of Mammalian Chromosome Architecture

AU - Krietenstein, Nils

AU - Abraham, Sameer

AU - Venev, Sergey V

AU - Abdennur, Nezar

AU - Gibcus, Johan

AU - Hsieh, Tsung-Han S

AU - Parsi, Krishna Mohan

AU - Yang, Liyan

AU - Maehr, René

AU - Mirny, Leonid A

AU - Dekker, Job

AU - Rando, Oliver J

PY - 2020/5/7

Y1 - 2020/5/7

N2 - Over the past decade, 3C-related methods have provided remarkable insights into chromosome folding in vivo. To overcome the limited resolution of prior studies, we extend a recently developed Hi-C variant, Micro-C, to map chromosome architecture at nucleosome resolution in human ESCs and fibroblasts. Micro-C robustly captures known features of chromosome folding including compartment organization, topologically associating domains, and interactions between CTCF binding sites. In addition, Micro-C provides a detailed map of nucleosome positions and localizes contact domain boundaries with nucleosomal precision. Compared to Hi-C, Micro-C exhibits an order of magnitude greater dynamic range, allowing the identification of ∼20,000 additional loops in each cell type. Many newly identified peaks are localized along extrusion stripes and form transitive grids, consistent with their anchors being pause sites impeding cohesin-dependent loop extrusion. Our analyses comprise the highest-resolution maps of chromosome folding in human cells to date, providing a valuable resource for studies of chromosome organization.

AB - Over the past decade, 3C-related methods have provided remarkable insights into chromosome folding in vivo. To overcome the limited resolution of prior studies, we extend a recently developed Hi-C variant, Micro-C, to map chromosome architecture at nucleosome resolution in human ESCs and fibroblasts. Micro-C robustly captures known features of chromosome folding including compartment organization, topologically associating domains, and interactions between CTCF binding sites. In addition, Micro-C provides a detailed map of nucleosome positions and localizes contact domain boundaries with nucleosomal precision. Compared to Hi-C, Micro-C exhibits an order of magnitude greater dynamic range, allowing the identification of ∼20,000 additional loops in each cell type. Many newly identified peaks are localized along extrusion stripes and form transitive grids, consistent with their anchors being pause sites impeding cohesin-dependent loop extrusion. Our analyses comprise the highest-resolution maps of chromosome folding in human cells to date, providing a valuable resource for studies of chromosome organization.

KW - Animals

KW - CCCTC-Binding Factor/metabolism

KW - Cells, Cultured

KW - Chromatin/chemistry

KW - Chromosomes, Human/ultrastructure

KW - Chromosomes, Mammalian/ultrastructure

KW - Embryonic Stem Cells/cytology

KW - Fibroblasts/cytology

KW - Humans

KW - Male

KW - Mammals/genetics

KW - Nucleosomes/metabolism

KW - Signal-To-Noise Ratio

U2 - 10.1016/j.molcel.2020.03.003

DO - 10.1016/j.molcel.2020.03.003

M3 - Journal article

C2 - 32213324

SN - 1097-2765

VL - 78

SP - 554-565.e7

JO - Molecular Cell

JF - Molecular Cell

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ER -