Genome-wide histone acetylation data improve prediction of mammalian transcription factor binding sites

Ramsey, Stephen A.; Knijnenburg, Theo; Kennedy, Kathleen A.; Zak, Daniel E.; Gilchrist, Mark; Gold, Elizabeth S.; Johnson, Carrie D.; Lampano, Aaron E.; Navarro, Garnet; Stolyar, Tetyana; Aderem, Alan; Shmulevich, Ilya

doi:10.1093/bioinformatics/btq405

Cited by 64 publications

(65 citation statements)

References 16 publications

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“…Unexpectedly, we noticed that BRD4 and histone acetylation existed in overlapping, yet largely distinct patterns (Figure 1A–B). Histone acetylation was found preferentially on nucleosomes that flank a nucleosome-depleted site, in a characteristic ‘valley’ of acetylation at enhancers and promoters (Ramsey et al, 2010). In contrast, BRD4 was enriched as a single peak, with its summit coinciding with the local minimum of both histone acetylation and overall histone density (Figure 1A–B).…”

Section: Resultsmentioning

confidence: 99%

BET Bromodomain Inhibition Suppresses the Function of Hematopoietic Transcription Factors in Acute Myeloid Leukemia

et al. 2015

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Summary The bromodomain and extraterminal (BET) protein BRD4 is a validated drug target in leukemia, yet its regulatory function in this disease is not well understood. Here, we show that BRD4 chromatin occupancy in acute myeloid leukemia closely correlates with the hematopoietic transcription factors (TFs) PU.1, FLI1, ERG, C/EBPα, C/EBPβ, and MYB at nucleosome-depleted enhancer and promoter regions. We provide evidence that these TFs, in conjunction with the lysine acetyltransferase activity of p300/CBP, facilitate BRD4 recruitment to their occupied sites to promote transcriptional activation. Chemical inhibition of BET bromodomains was found to suppress the functional output each hematopoietic TF, thereby interfering with essential lineage-specific transcriptional circuits in this disease. These findings reveal a chromatin-based signaling cascade comprised of hematopoietic TFs, p300/CBP, and BRD4 that supports leukemia maintenance and is suppressed by BET bromodomain inhibition.

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Section: Resultsmentioning

confidence: 99%

BET Bromodomain Inhibition Suppresses the Function of Hematopoietic Transcription Factors in Acute Myeloid Leukemia

et al. 2015

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“…As we found little evidence for changes in these histone modifications between diets, we used the set of significant ChIP-seq regions in CD livers for our analyses. We searched each dataset for histone “valleys,” or regions between peaks of local modification enrichment where histones are depleted and where regulators likely bind (Figure 3A) (Ramsey et al, 2010; Wamstad et al, 2012). We merged these discovered valleys into one set of 123,974 total loci and scanned the underlying genomic sequences for matches to a set of 1,588 DNA-binding motifs that map to at least one human or mouse transcriptional regulator (Figure 3B).…”

Section: Resultsmentioning

confidence: 99%

Hepatic Dysfunction Caused by Consumption of a High-Fat Diet

Soltis

Kennedy

et al. 2017

Cell Reports

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SUMMARY Obesity is a major human health crisis that promotes insulin resistance and, ultimately, type 2 diabetes. The molecular mechanisms that mediate this response occur across many highly complex biological regulatory levels that are incompletely understood. Here, we present a comprehensive molecular systems biology study of hepatic responses to high-fat feeding in mice. We interrogated diet-induced epigenomic, transcriptomic, proteomic, and metabolomic alterations using high-throughput omic methods and used a network modeling approach to integrate these diverse molecular signals. Our model indicated that disruption of hepatic architecture and enhanced hepatocyte apoptosis are among the numerous biological processes that contribute to early liver dysfunction and low-grade inflammation during the development of diet-induced metabolic syndrome. We validated these model findings with additional experiments on mouse liver sections. In total, we present an integrative systems biology study of diet-induced hepatic insulin resistance that uncovered molecular features promoting the development and maintenance of metabolic disease.

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“…Within any given SE, enriched TF binding sites were determined at putative nucleosome free regions (valleys) flanked by high levels of H3K27ac. Valleys were calculated using an algorithm adapted from Ramsey et al, 2010 13 . In these regions, we searched for enriched TF binding sites using the FIMO59 algorithm with TF position weight matrices defined in the TRANSFAC database 24 .…”

Section: Methodsmentioning

confidence: 99%

“…Regulation of cell type specific gene expression is often dominated by only a small number of core transcription factors (TFs) out of the hundreds expressed within a given cell type 13 . While many significant TF motifs were enriched across shared enhancers of ependymoma, such as FOSL1, FOSL2, SOX9, RFX2, and SOX2 (Fig.…”

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confidence: 99%

Therapeutic targeting of ependymoma as informed by oncogenic enhancer profiling

Mack¹,

Pajtler

Chávez

et al. 2017

Nature

182

218

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SUMMARY Genomic sequencing has driven precision-based oncology therapy; however, genetic drivers remain unknown or non-targetable for many malignancies, demanding alternative approaches to identify therapeutic leads. Ependymomas are chemotherapy-resistant brain tumours, which, despite genomic sequencing, lack effective molecular targets. Intracranial ependymomas are segregated based on anatomical location – supratentorial region (ST) or posterior fossa (PF) – and further divided into distinct molecular subgroups that reflect differences in age of onset, gender predominance, and response to therapy1–3. The most common and aggressive subgroup, Posterior Fossa Ependymoma Group A (PF-EPN-A), occurs in young children and appears to lack recurrent somatic mutations2. Conversely, Posterior Fossa Ependymoma Group B (PF-EPN-B) tumours display frequent large-scale copy number gains and losses yet favourable clinical outcomes1,3. Greater than 70% of supratentorial ependymomas are defined by highly recurrent gene fusions in the NFκB subunit RELA (ST-EPN-RELA), and less frequently involve fusion of the gene encoding the transcriptional activator YAP1 (ST-EPN-YAP1).1,3,4 Subependymomas, a distinct histologic variant, can also be found within the ST and PF compartments accounting for the majority of tumours in the molecular subgroups ST-EPN-SE and PF-EPN-SE, respectively1. Here, we mapped active chromatin landscapes in 42 primary ependymomas in two non-overlapping primary ependymoma cohorts with the goal of identifying essential super enhancer associated genes on which tumour cells were dependent. Enhancer regions revealed putative oncogenes, molecular targets, and pathways, which when subjected to small molecule inhibitor or shRNA treatment, diminished proliferation of patient-derived neurospheres and increased survival in mouse models of ependymomas. Through profiling of transcriptional enhancers, our study provides a framework for target and drug discovery in other cancers recalcitrant to therapeutic development because of their lack of known genetic drivers.

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Genome-wide histone acetylation data improve prediction of mammalian transcription factor binding sites

Cited by 64 publications

References 16 publications

BET Bromodomain Inhibition Suppresses the Function of Hematopoietic Transcription Factors in Acute Myeloid Leukemia

BET Bromodomain Inhibition Suppresses the Function of Hematopoietic Transcription Factors in Acute Myeloid Leukemia

Hepatic Dysfunction Caused by Consumption of a High-Fat Diet

Therapeutic targeting of ependymoma as informed by oncogenic enhancer profiling

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