Transcriptional refractoriness is dependent on core promoter architecture

Cesbron, François; Oehler, Michael; Ha, Nati; Sancar, Gencer; Brunner, Michael

doi:10.1038/ncomms7753

Cited by 30 publications

(78 citation statements)

References 70 publications

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“…Third, while the presence of NELF marks a paused gene, it is possible that it is involved only in a portion of individual transcription initiation events. We suggest that availability of NELF, or a functionally similar factor, may explain recently described events such as transcriptional bursts (Singh et al 2010; Bothma et al 2014) or transcriptional ‘memory’ (Cesbron et al 2015). Consistent with its involvement in regulation, NELF levels are altered in cancer cells (Sun et al 2008).…”

Section: Regulation Of Early Elongation: a Checkpoint On Every Gene?mentioning

confidence: 68%

RNA polymerase II pausing as a context-dependent reader of the genome

Scheidegger

Nechaev

2016

Biochem. Cell Biol.

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Summary The RNA polymerase II (Pol II) transcribes all mRNA genes in eukaryotes and is among the most highly regulated enzymes in the cell. The classic model of mRNA gene regulation involves recruitment of the RNA polymerase to gene promoters in response to environmental signals. Higher eukaryotes have an additional ability to generate multiple cell types. This extra level of regulation enables each cell to interpret the same genome by committing to one of the many possible transcription programs and executing it in a precise and robust manner. Whereas multiple mechanisms are implicated in cell type-specific transcriptional regulation, how one genome can give rise to distinct transcriptional programs and what mechanisms activate and maintain the appropriate program in each cell remains unclear. This review focuses on the process of promoter-proximal Pol II pausing during early transcription elongation as a key step in context-dependent interpretation of the metazoan genome. We highlight aspects of promoter-proximal Pol II pausing, including its interplay with epigenetic mechanisms, that may enable cell type-specific regulation, and emphasize some of the pertinent questions that remain unanswered and open for investigation.

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Section: Regulation Of Early Elongation: a Checkpoint On Every Gene?mentioning

confidence: 68%

RNA polymerase II pausing as a context-dependent reader of the genome

Scheidegger

Nechaev

2016

Biochem. Cell Biol.

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“…As the enzymatic activity of Pol II was not compromised by THL, we performed chromatin immunoprecipitation (ChIP) of Pol II phosphorylated at Ser5 of the C-terminal domain repeats (Pol II S5-P) to assess whether THL affects recruitment of Pol II and initiation of transcription at selected promoters 25 . Quantification of Pol II S5-P occupancy by ChIP-PCR correlated with the results of the RNAseq analysis: although Pol II S5-P enrichment at the promoter regions of frq , vvd, and actin decreased significantly in the presence of THL, recruitment of Pol II to hsp98 and hsp60 increased (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…The RNA polymerase II ChIP was performed as described 25 . Briefly, light grown cultures were incubated for 40 min in the presence of DMSO and 50 μM THL, respectively.…”

Section: Methodsmentioning

confidence: 99%

“…Briefly, light grown cultures were incubated for 40 min in the presence of DMSO and 50 μM THL, respectively. Samples were cross-linked for 10 min with 1% formaldehyde and subjected to ChIP with antibodies against Pol II Ser5-P 25 . Precipitated DNA was quantified by qRT–PCR with promoter specific probes: actin: F: tatcatgggcacaagctgat, R: cttacccattgtcgatgacg, Probe: 6-FAM - tgcgttcccgccaacagaag - TAMRA; vvd: F: ttagcctttgccagttaggg, R: tgttggtagggtattatgatggttt, Probe: UPL #41; hsp98: F: cattttgctggtccttgctc, R: cccgttcatctggcagtc, Probe: UPL #14; hsp60: F: gcgttgaccagagcttcc, R: ggatcgtaccttgtgagcaaa, Probe: UPL #3.…”

Section: Methodsmentioning

confidence: 99%

“…Pelleted nuclei were sonicated in 300 μl IP buffer supplemented with 0.8% SDS (30 s on/30 s off cycles for 40 min) using a Bioruptor (Diagenode Inc.). The chromatin (equivalent of 5×10 5 cells) was then incubated overnight at 4°C with 4 μl affinity purified anti-Pol II Ser2-P antibody 25 and precipitated with salmon sperm DNA blocked protein A-sepharose beads. Beads were washed 5 times with IP buffer and co-precipitated DNA was recovered by boiling for 10 min in 10% Chelex slurry (Bio-Rad) and treatment with Proteinase K (150 μg/ml, NEB) at 55°C for 30 min.…”

Section: Methodsmentioning

confidence: 99%

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Thiolutin is a zinc chelator that inhibits the Rpn11 and other JAMM metalloproteases

et al. 2017

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Thiolutin is a disulfide-containing antibiotic and anti-angiogenic compound produced by Streptomyces. Its biological targets are not known. We show that reduced thiolutin is a zinc-chelator that inhibits the JAB1/MPN/Mov34 (JAMM) domain-containing metalloprotease Rpn11, a de-ubiquinating enzyme of the 19S proteasome. Thiolutin also inhibits the JAMM metalloproteases Csn5, the deneddylase of the COP9 signalosome, Associated-molecule-with-the-SH3-Domain-of-STAM (AMSH), which regulates ubiquitin-dependent sorting of cell-surface receptors, and Brcc36, a K63-specific deubiquitnase of BRCC36-containing isopeptidase complex (BRISC) and BRCA1-BRCA2-containing complex (BRCC). We provide evidence that other dithiolopyrrolones also function as inhibitors of JAMM metalloproteases.

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Systems Biological Applications for Fungal Gene Expression

Akçapınar¹,

Sezerman

2016

Fungal Biology

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Transcriptional refractoriness is dependent on core promoter architecture

Cited by 30 publications

References 70 publications

RNA polymerase II pausing as a context-dependent reader of the genome

RNA polymerase II pausing as a context-dependent reader of the genome

Thiolutin is a zinc chelator that inhibits the Rpn11 and other JAMM metalloproteases

Systems Biological Applications for Fungal Gene Expression

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