Dynamic Reorganization of Extremely Long-Range Promoter-Promoter Interactions between Two States of Pluripotency

Joshi, Onkar; Wang, Shuang-Yin; Кузнецова, Т. Н.; Atlasi, Yaser; Peng, Tianran; Fabre, Pierre J.; Habibi, Ehsan; Shaik, Jani; Saeed, Sadia; Handoko, Lusy; Richmond, Todd; Spivakov, Mikhail; Burgess, Daniel L.; Stunnenberg, Hendrik G.

doi:10.1016/j.stem.2015.11.010

Cited by 192 publications

(217 citation statements)

References 40 publications

(68 reference statements)

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“…At active/enhancer regions, the Mediator complex is thought to sustain long-range interactions with associated promoters and could account for part of these CTCF-independent interactions (Phillips-Cremins et al 2013). At repressed regions, the PRC1 and PRC2 complex were shown to mediate long-range interactions and could account for the homotypic bridging of H3K27me3-rich chromatin regions (Denholtz et al 2013;Joshi et al 2015;Schoenfelder et al 2015). The controlled spatial clustering of repressed or active regions, analogous to the domain-wide clustering of A and B compartments on a larger scale (Lieberman-Aiden et al 2009), could be seen as another layer of gene regulation.…”

Section: Discussionmentioning

confidence: 99%

Characterization of hundreds of regulatory landscapes in developing limbs reveals two regimes of chromatin folding

et al. 2016

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Complex regulatory landscapes control the pleiotropic transcriptional activities of developmental genes. For most genes, the number, location, and dynamics of their associated regulatory elements are unknown. In this work, we characterized the three-dimensional chromatin microarchitecture and regulatory landscape of 446 limb-associated gene loci in mouse using Capture-C, ChIP-seq, and RNA-seq in forelimb, hindlimb at three developmental stages, and midbrain. The fine mapping of chromatin interactions revealed a strong preference for functional genomic regions such as repressed or active domains. By combining chromatin marks and interaction peaks, we annotated more than 1000 putative limb enhancers and their associated genes. Moreover, the analysis of chromatin interactions revealed two regimes of chromatin folding, one producing interactions stable across tissues and stages and another one associated with tissue and/or stage-specific interactions. Whereas stable interactions associate strongly with CTCF/RAD21 binding, the intensity of variable interactions correlates with changes in underlying chromatin modifications, specifically at the viewpoint and at the interaction site. In conclusion, this comprehensive data set provides a resource for the characterization of hundreds of limb-associated regulatory landscapes and a framework to interpret the chromatin folding dynamics observed during embryogenesis.

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Section: Discussionmentioning

confidence: 99%

Characterization of hundreds of regulatory landscapes in developing limbs reveals two regimes of chromatin folding

et al. 2016

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“…In this respect, the loss of PRC2 function disrupts long range interactions [53,54], but does not affect mammalian TAD formation.…”

Section: Polycomb Group Complexes Regulate Chromatin At Different Scalesmentioning

confidence: 99%

Switch-Like Roles for Polycomb Proteins from Neurodevelopment to Neurodegeneration

et al. 2017

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Polycomb Group (PcG) proteins are best-known for maintaining repressive or active chromatin states that are passed on across multiple cell divisions, and thus sustain long-term memory of gene expression. PcG proteins engage different, partly gene-and/or stage-specific, mechanisms to mediate spatiotemporal gene expression during central nervous system development. In the course of this, PcG proteins bind to various cis-regulatory sequences (e.g., promoters, enhancers or silencers) and coordinate, as well the interactions between distantly separated genomic regions to control chromatin function at different scales ranging from compaction of the linear chromatin to the formation of topological hubs. Recent findings show that PcG proteins are involved in switch-like changes in gene expression states of selected neural genes during the transition from multipotent to differentiating cells, and then to mature neurons. Beyond neurodevelopment, PcG proteins sustain mature neuronal function and viability, and prevent progressive neurodegeneration in mice. In support of this view, neuropathological findings from human neurodegenerative diseases point to altered PcG functions. Overall, improved insight into the multiplicity of PcG functions may advance our understanding of human neurodegenerative diseases and ultimately pave the way to new therapies.

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“…Klf1 and pluripotency factor networks (7,9). Similarly, loci associated with Polycomb proteins and the repressive chromatin modification H3K27me3 tend to cluster together (10). Artificial tethering of TFs via the lac integration cassette has further corroborated this observation.…”

Section: Spatial Clustering Of Co-regulated Genesmentioning

confidence: 80%

Dynamic chromatin organization: Role in development and disease

Кузнецова

Stunnenberg

2016

The International Journal of Biochemistry & Cell Biology

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Dynamic Reorganization of Extremely Long-Range Promoter-Promoter Interactions between Two States of Pluripotency

Cited by 192 publications

References 40 publications

Characterization of hundreds of regulatory landscapes in developing limbs reveals two regimes of chromatin folding

Characterization of hundreds of regulatory landscapes in developing limbs reveals two regimes of chromatin folding

Switch-Like Roles for Polycomb Proteins from Neurodevelopment to Neurodegeneration

Dynamic chromatin organization: Role in development and disease

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