Ch
            <scp>IP</scp>
            ‐Atlas: a data‐mining suite powered by full integration of public Ch
            <scp>IP</scp>
            ‐seq data

Oki, Shinya; Ohta, Toshio; Shioi, Go; Hatanaka, Hideki; Ogasawara, Osamu; Okuda, Yoshihiro; Kawaji, Hideya; Nakaki, Ryo; Sese, Jun; Meno, Chikara

doi:10.15252/embr.201846255

Cited by 595 publications

(478 citation statements)

References 37 publications

(50 reference statements)

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“…The presence of the peak, located on chromosome 11, positions: 119,037,091-119,037,351 (genome version hg19) was reported in meta-analysis performed by Nguyen et al [32]. The p53 ChIP-Seq peaks identified by others in this region and publically available through ChIP-Atlas tool [33] are visualized in supplementary Fig. S2.…”

Section: Ectopic Expression Of P53 Upregulates Nlrx1 and Nlrp1 Promotersmentioning

confidence: 71%

“…B. Genome browser (IGV) views of p53 binding peak at the exon1/intron1 border of IL7 gene. Using ChIP-Atlas tool [33] we imported publically available coverage tracks from four ChIP-Seq experiments aimed at finding p53 binding sites in MCF-7 cell line exposed to ionizing radiation and Nutlin (sample ID SRX2924018), SAOS-2 cell line ectopically expressing wild-type p53 (sample ID SRX016980), SAOS-2 ectopically expressing pair of engineered p53 molecules with strong cooperative binding of p53 monomers [31] (sample ID ERX181467) or in MCF7 cells treated with Nutlin (sample ID SRX2060922). C. Measurement of relative IL7 mRNA levels in A549 cells exposed to indicated substances or combination treatments for 30 h. D. Relative IL7 mRNA levels in p53 knockdown A549 cells (p53-SH), and control cells (Con-SH), exposed to A + N or CPT for 30 h (p values from three repeats calculated by Student's t-test).…”

Section: Discussionmentioning

confidence: 99%

“…To find out if A + N treatment can induce genes coding for immunerelated extracellular molecules we searched for p53 ChIP-Seq peaks in genes encoding various cytokines and chemokines. Interestingly, using ChIP-Atlas [33], we found p53 ChIP-Seq peak at the exon 1/intron 1 border of interleukin-7 gene (Fig. 12B).…”

Section: Cells Exposed To a + N Can Modulate Their Environmentmentioning

confidence: 92%

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Synergistic activation of p53 by actinomycin D and nutlin-3a is associated with the upregulation of crucial regulators and effectors of innate immunity

Krześniak

Zajkowicz

Gdowicz-Kłosok

et al. 2020

Cellular Signalling

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A B S T R A C TActinomycin D and nutlin-3a (A + N) activate p53, partly through induction of phosphorylation on Ser392. The death of A549 cells induced by A + N morphologically resembles inflammation-inducing pyroptosis -cell destruction triggered by activated caspase-1. The treatment with A + N (or camptothecin) strongly upregulated caspase-1 and its two activators: IFI16 and NLRP1, however, caspase-1 activation was not detected. A549 cells may have been primed for pyroptosis, with the absence of a crucial trigger. The investigation of additional innate immunity elements revealed that A + N (or camptothecin) stimulated the expression of NLRX1, STING (stimulator of interferon genes) and two antiviral proteins, IFIT1 and IFIT3. IFI16 and caspase-1 are coded by p53regulated genes which led us to investigate regulation of NLRP1, NLRX1, STING, IFIT1 and IFIT3 in p53-dependent mode. The upregulation of NLRP1, NLRX1 and STING was attenuated in p53 knockdown cells. The upsurge of the examined genes, and activation of p53, was inhibited by C16, an inhibitor of PKR kinase. PKR was tested due to its ability to phosphorylate p53 on Ser392. Surprisingly, C16 was active even in PKR knockdown cells. The ability of C16 to prevent activation of p53 and expression of innate immunity genes may be the source of its strong anti-inflammatory action. Moreover, cells exposed to A + N can influence neighboring cells in paracrine fashion, for instance, they shed ectodomain of COL17A1 protein and induce, in p53-dependent mode, the expression of gene for interleukin-7. Further, the activation of p53 also spurred the expression of SOCS1, an inhibitor of interferon triggered STAT1-dependent signaling. We conclude that, stimulation of p53 primes cells for the production of interferons (through upregulation of STING), and may activate negative-feedback within this signaling system by enhancing the production of SOCS1.

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Section: Ectopic Expression Of P53 Upregulates Nlrx1 and Nlrp1 Promotersmentioning

confidence: 71%

Section: Discussionmentioning

confidence: 99%

Section: Cells Exposed To a + N Can Modulate Their Environmentmentioning

confidence: 92%

See 1 more Smart Citation

Synergistic activation of p53 by actinomycin D and nutlin-3a is associated with the upregulation of crucial regulators and effectors of innate immunity

Krześniak

Zajkowicz

Gdowicz-Kłosok

et al. 2020

Cellular Signalling

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“…A set of genes where POU5F1 binds in the vicinity of the TSS in primed hESCs were identified using ChIPseq data 35 . An initial set of 11 hESC samples (SRX017276, SRX021069, SRX021071, SRX1053369, SRX1053370, SRX1053378, SRX1053379, SRX266859, SRX702065, SRX702066, SRX702069) were collected from CHiP-Atlas 35 by filtering with POU5F1 as antigen and a distance from TSS as 1 kb. For the remaining samples hierarchical clustering of the euclidean distance all samples binding scores across all genes compared to each other was done.…”

Section: Gene Regulatory Network Analysis -Selection Of Pou5f1 Targetsmentioning

confidence: 99%

Combined mRNA and protein single cell analysis in a dynamic cellular system using SPARC

Reimegård

Danielsson

Tarbier

et al. 2019

Preprint

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Combined measurements of mRNA and protein expression in single cells enables in-depth analysis of cellular states. We present single-cell protein and RNA co-profiling (SPARC), an approach to simultaneously measure global mRNA and large sets of intracellular protein in individual cells. Using SPARC, we show that mRNA expression fails to accurately reflect protein abundance at the time of measurement in human embryonic stem cells, although the direction of changes of mRNA and protein expression are in agreement during cellular differentiation. Moreover, protein levels of transcription factors better predict their downstream effects than do the corresponding transcripts. We further show that changes of the balance between protein and mRNA expression levels can be applied to infer expression kinetic trajectories, revealing future states of individual cells. Finally, we highlight that mRNA expression may be more varied among cells than levels of the corresponding proteins. Overall, our results demonstrate that mRNA and protein measurements in single cells provide different and complementary information regarding cell states. Accordingly, SPARC can offer valuable insights in gene expression programs of single cells.

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“…To further confirm the functions of the TFBS, we searched the interaction of transcriptional factors with the enhancer on ChIP-Atlas (http://chip-atlas.org). 18 We found a strong peak overlapping the enhancer in a ChIP-seq of LHX6 performed on E11.5 maxillary arch cells ( Figure 4M). 19 The peak is flanked by a H3K27ac peak detected in the E11.5 mouse maxillary arch, 20 suggesting the binding site is located in an active enhancer.…”

Section: Two Six1 Enhancers Act Synergistically In the Maxillary Prmentioning

confidence: 88%

Cis‐control of Six1 expression in neural crest cells during craniofacial development

Rao

Zhang

et al. 2019

Developmental Dynamics

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Background Six1 is a transcriptional factor that plays an important role in embryonic development. Mouse and chick embryos deficient for Six1 have multiple craniofacial anomalies in the facial bones and cartilages. Multiple Six1 enhancers have been identified, but none of them has been reported to be active in the maxillary and mandibular process. Results We studied two Six1 enhancers in the chick neural crest tissues during craniofacial development. We showed that two evolutionarily conserved enhancers, Six1E1 and Six1E2, act synergistically. Neither Six1E1 nor Six1E2 alone can drive enhancer reporter signal in the maxillary or mandibular processes. However, their combination, Six1E, showed robust enhancer activity in these tissues. Similar reporter signal can also be driven by the mouse homolog of Six1E. Mutations of multiple conserved transcriptional factor binding sites altered the enhancer activity of Six1E, especially mutation of the LIM homeobox binding site, dramatically reduced the enhancer activity, implying that the Lhx protein family be an important regulator of Six1 expression. Conclusion This study, for the first time, described the synergistic activation of two Six1 enhancers in the maxillary and mandibular processes and will facilitate more detailed studies of the regulation of Six1 in craniofacial development.

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Ch IP ‐Atlas: a data‐mining suite powered by full integration of public Ch IP ‐seq data

Cited by 595 publications

References 37 publications

Synergistic activation of p53 by actinomycin D and nutlin-3a is associated with the upregulation of crucial regulators and effectors of innate immunity

Synergistic activation of p53 by actinomycin D and nutlin-3a is associated with the upregulation of crucial regulators and effectors of innate immunity

Combined mRNA and protein single cell analysis in a dynamic cellular system using SPARC

Cis‐control of Six1 expression in neural crest cells during craniofacial development

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