Genetic Control of Chromatin States in Humans Involves Local and Distal Chromosomal Interactions

Grubert, Fabian; Zaugg, Judith B.; Kasowski, Maya; Ursu, Oana; Spacek, Damek V.; Ar, Martin; Greenside, Peyton G.; Srivas, Rohith; Phanstiel, Doug; Pękowska, Aleksandra; Heidari, Nastaran; Euskirchen, Ghia; Huber, Wolfgang; Pritchard, Jonathan K.; Bustamante, Carlos D.; Steinmetz, Lars M.; Kundaje, Anshul; Snyder, M

doi:10.1016/j.cell.2015.07.048

Cited by 308 publications

(402 citation statements)

References 40 publications

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“…In line with this, gene silencing on the inactive X chromosome in female mammalian cells was shown to also occur at the level of TADs, and gene clusters of escapees that do not become silenced correlate with TADs (Marks et al 2015). Further strong evidence for TADs being the functional units of the genome came from two recent studies that established the existence of the long-range impact of genetic variation on histone modifications elsewhere on chromosomes: Both studies showed that such communication takes place in the context of TADs (Grubert et al 2015;Waszak et al 2015). TADs are formed during early G1 of the cell cycle, concomitant with the establishment of the replication timing program (Dileep et al 2015), and TAD boundaries often coincide with replication domain boundaries (Pope et al 2014).…”

Section: Tads and Sub-tadsmentioning

confidence: 96%

The second decade of 3C technologies: detailed insights into nuclear organization

2016

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The relevance of three-dimensional (3D) genome organization for transcriptional regulation and thereby for cellular fate at large is now widely accepted. Our understanding of the fascinating architecture underlying this function is based on microscopy studies as well as the chromosome conformation capture (3C) methods, which entered the stage at the beginning of the millennium. The first decade of 3C methods rendered unprecedented insights into genome topology. Here, we provide an update of developments and discoveries made over the more recent years. As we discuss, established and newly developed experimental and computational methods enabled identification of novel, functionally important chromosome structures. Regulatory and architectural chromatin loops throughout the genome are being cataloged and compared between cell types, revealing tissue invariant and developmentally dynamic loops. Architectural proteins shaping the genome were disclosed, and their mode of action is being uncovered. We explain how more detailed insights into the 3D genome increase our understanding of transcriptional regulation in development and misregulation in disease. Finally, to help researchers in choosing the approach best tailored for their specific research question, we explain the differences and commonalities between the various 3C-derived methods.

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Section: Tads and Sub-tadsmentioning

confidence: 96%

The second decade of 3C technologies: detailed insights into nuclear organization

2016

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“…Genomewide association studies showed several events of single nucleotide variants (SNVs) occurring at enhancers of disease-causing genes. 114,115 Using the knowledge revealed so far about the role of SNVs or mutations in gene deregulation and disease susceptibility, it could be hypothesized that such alterations may be causative for low CEBPA expression in these CEBPA low AML subgroups. The application of DNA custom capture sequencing in large AML cohorts would be a potential tool to reveal mutations or SNVs that may be occurring in the CEBPA locus.…”

Section: Hijacking Of the Cebpa Locus By Potential Oncoproteinsmentioning

confidence: 99%

Expression and regulation of C/EBPα in normal myelopoiesis and in malignant transformation

Avellino

Delwel

2017

Blood

124

110

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One of the most studied transcription factors in hematopoiesis is the leucine zipper CCAAT-enhancer binding protein α (C/EBPα), which is mainly involved in cell fate decisions for myeloid differentiation. Its involvement in acute myeloid leukemia (AML) is diverse, with patients frequently exhibiting mutations, deregulation of gene expression, or alterations in the function of C/EBPα. In this review, we emphasize the importance of C/EBPα for neutrophil maturation, its role in myeloid priming of hematopoietic stem and progenitor cells, and its indispensable requirement for AML development. We discuss that mutations in the open reading frame of CEBPA lead to an altered C/EBPα function, affecting the expression of downstream genes and consequently deregulating myelopoiesis. The emerging transcriptional mechanisms of CEBPA are discussed based on recent studies. Novel insights on how these mechanisms may be deregulated by oncoproteins or mutations/variants in CEBPA enhancers are suggested in principal to reveal novel mechanisms of how CEBPA is deregulated at the transcriptional level.

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“…One of the most widely used methods to detect higherorder chromatin structure is the chromosome conformation capture (3C) family of techniques. 146,153,160 Chromatin immunoprecipitation sequencing (ChIP-seq), micrococcal nuclease sequencing (MNase-seq), and chromatin immunoprecipitation exonuclease (ChIP-exo) methodologies provide information over the »1-150 bp length scale, allowing for analysis of nucleosome fiber folding 149,[161][162][163][164] . While these types of approaches provide information on populations of cells, single-cell approaches have now become feasible.…”

Section: Does Nuclear Morphology Affect Chromatin Organization?mentioning

confidence: 99%

Recent advances in understanding nuclear size and shape

Mukherjee

Chen

Levy

2016

Nucleus

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Size and shape are important aspects of nuclear structure. While normal cells maintain nuclear size within a defined range, altered nuclear size and shape are associated with a variety of diseases. It is unknown if altered nuclear morphology contributes to pathology, and answering this question requires a better understanding of the mechanisms that control nuclear size and shape. In this review, we discuss recent advances in our understanding of the mechanisms that regulate nuclear morphology, focusing on nucleocytoplasmic transport, nuclear lamins, the endoplasmic reticulum, the cell cycle, and potential links between nuclear size and size regulation of other organelles. We then discuss the functional significance of nuclear morphology in the context of early embryonic development. Looking toward the future, we review new experimental approaches that promise to provide new insights into mechanisms of nuclear size control, in particular microfluidic-based technologies, and discuss how altered nuclear morphology might impact chromatin organization and physiology of diseased cells.

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Genetic Control of Chromatin States in Humans Involves Local and Distal Chromosomal Interactions

Cited by 308 publications

References 40 publications

The second decade of 3C technologies: detailed insights into nuclear organization

The second decade of 3C technologies: detailed insights into nuclear organization

Expression and regulation of C/EBPα in normal myelopoiesis and in malignant transformation

Recent advances in understanding nuclear size and shape

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