NELF and DSIF cause promoter proximal pausing on the<i>hsp70</i>promoter in<i>Drosophila</i>

Wu, Chwen Huey; Yamaguchi, Yuki; Benjamin, Lawrence R.; Horvat-Gordon, Maria; Washinsky, Jodi; Enerly, Espen; Larsson, Jonas; Lambertsson, Andrew; Handa, Hiroshi; Gilmour, David S.

doi:10.1101/gad.1091403

Cited by 279 publications

(292 citation statements)

References 65 publications

(96 reference statements)

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“…Some, but not all, activators have been shown to interact with P-TEFb, so other mechanisms of P-TEFb recruitment need to be considered 26 . The transition into productive elongation seems to correlate with the loss of NELF from the promoter 27 . In contrast, DSIF remains associated with productively elongating Pol II and is thought to have a positive role after escape from the pause 2,28 .…”

Section: Molecular Imaging Of Proteins On Genes In Vivomentioning

confidence: 99%

“…Using ChIP assays, both DSIF and NELF were found to be located along with paused Pol II in the promoter-proximal regions of uninduced heat shock genes (Fig. 4) 2,27 . The P-TEFb kinase is recruited to active genes where it overcomes the negative effects through its kinase activity, which can phosphorylate DSIF, NELF and Ser 2 residues of the carboxy-terminal domain of the largest subunit of Pol II 2,26 .…”

Section: Molecular Imaging Of Proteins On Genes In Vivomentioning

confidence: 99%

“…Whereas these melted residues tend to cluster in the region of 20-50 base pairs and highly correlate with paused Pol II, the pattern of reactivity can be influenced by other proteins either protecting or altering the reactivity of T residues. Additional signatures can be detected by ChIP assays and include the presence of NELF, and Ser 5-but not Ser 2-phosphorylated carboxy-terminal domain of the largest subunit (RpII215) of Pol II 20,27 .…”

Section: Defining a Pol II As 'Promoter Paused'mentioning

confidence: 99%

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Imaging Drosophila gene activation and polymerase pausing in vivo

Lis

2007

Nature

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Since the early 1960s, imaging studies of Drosophila sp. polytene chromosomes have provided unique views of gene transcription in vivo. The dramatic changes in chromatin structure that accompany gene activation can be visualized as chromosome puffs. Now, live-cell imaging techniques coupled with protein-DNA crosslinking assays on a genome-wide scale allow more detailed mechanistic questions to be addressed and are prompting the re-evaluation of models of transcription regulation in both Drosophila and mammals.D etermining the complete genome sequence of humans, Drosophila and other model higher eukaryotes was an important step in cataloguing the complete code that programmes the development and maintenance of multicellular organisms. A critical challenge that remains is to determine in molecular terms how this code is read and regulated in higher eukaryotes 1 . The regulation of transcription of the genome is a major mode by which an organism controls both its homeostasis and development. This regulation is executed mainly through the interactions of a plethora of transcription factor proteins and RNAs with each other and with DNA and associated histones 2 . These interactions then dictate when, where, and to what level specific genes are transcribed. Although biochemical and genetic approaches have identified many of the macromolecular players and their activities, a mechanistic understanding of how they operate in gene regulation can be guided and tested by direct imaging of these molecular interactions and the resulting biochemical processes in living cells.Two developments in the imaging of transcription factors at specific endogenous gene loci in vivo are providing new views of transcription mechanisms and regulation. One, currently specific to Drosophila, makes use of state-of-the-art optics combined with the natural amplification of signals in tissue containing polytene chromosomes, allowing investigation of molecular interactions and dynamics at specific loci in real time in living nuclei 3 . The other, although having a history in Drosophila 4-6 , is species-general and uses crosslinking in vivo-that is, chromatin immunoprecipitation (ChIP) assays and variants thereof-to produce a 'molecular image' of specific protein interactions and chromatin modifications with particular DNA sequences in the genome 7 . Here I describe how these optical and molecular imaging approaches are providing new insights into transcription and the rate-limiting steps in its regulation in multicellular organisms. In particular, recent genome-wide ChIP assays in Drosophila 8,9 and mammals 10 support a paradigm shift in gene regulation by indicating that control of transcription elongation by RNA polymerase II (Pol II) in a promoter-proximal pausing model (Box 1), rather than control of the recruitment or initiation of Pol II, is the rate-limiting step for a large fraction of highly regulated genes. Early insights from spread polytene nucleiOver the past several decades, Drosophila has provided extraordinary views of chromosome s...

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Section: Molecular Imaging Of Proteins On Genes In Vivomentioning

confidence: 99%

Section: Molecular Imaging Of Proteins On Genes In Vivomentioning

confidence: 99%

Section: Defining a Pol II As 'Promoter Paused'mentioning

confidence: 99%

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Imaging Drosophila gene activation and polymerase pausing in vivo

Lis

2007

Nature

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“…Rather, the positioned +1 nucleosome might be contributing to pol II pausing, which is consistent with other studies [34][35][36][37] . Other factors including NELF are likely to make significant contributions to pausing as well 30,38,39 .…”

Section: Rna Polymerase II Contacts the +1 Nucleosome And Pausesmentioning

confidence: 99%

Nucleosome organization in the Drosophila genome

Mavrich

Jiang

Ioshikhes

et al. 2008

Nature

656

690

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Comparative genomics of nucleosome positions provides a powerful means for understanding how the organization of chromatin and the transcription machinery co-evolve. Here we produce a high resolution reference map of H2A.Z and bulk nucleosome locations across the genome of the fly D. melanogaster, and compare it to that from the yeast S. cerevisiae. Like Saccharomyces, Drosophila nucleosomes are organized around active transcription start sites in a canonical −1, NFR (nucleosome-free region), +1 arrangement. However, Drosophila does not incorporate H2A.Z into the −1 nucleosome and does not bury its transcriptional start site in the +1 nucleosome. At thousands of genes, RNA polymerase II engages the +1 nucleosome and pauses. How the transcription initiation machinery contends with the +1 nucleosome appears to be fundamentally different between lower and higher eukaryotes.Knowledge of the precise location of nucleosomes in a genome is essential in order to understand the context in which chromosomal processes such as transcription and DNA replication operate. A common theme to emerge from recent genome-wide maps of nucleosome locations is a general deficiency of nucleosomes in promoter regions and an enrichment of certain histone modifications towards the 5′ end of genes [1][2][3][4][5][6][7] . A high resolution genomic map of nucleosome locations in the budding yeast S. cerevisiae has further revealed Correspondence and request for material should be addressed to B.F.P. (bfp2@psu.edu). * These authors contributed equally to this work.Author Information Sequence data deposition is through NCBI Trace Archives TI SRA000283, Sequencing Center = "CCGB", and microarray deposition through ArrayExpress, Accession numbers E-MEXP-1515 and -1519. Reprints and permissions information is available at www.nature.com/reprints. The authors declare no competing financial interest.Author Contributions T.M. prepared and purified the nucleosomes including Pol II-bound nucleosomes; C.J. analyzed the nucleosome mapping data and its relationship to other genomic features; I.P.I. performed computational analyses related to nucleosome positioning sequences; X.L. conducted ChIP-chip on Pol II; B.J.V. conducted ChIP-chip on nucleosome-Pol II interactions; S.J.Z. provided bioinformatics support; L.T. constructed libraries and sequenced nucleosomal DNA; J.Q. mapped sequencing reads to the yeast genome; RG provided H2A.Z antibodies; SCS directed the DNA sequencing phase; DSG directed embryo preparations and helped interpret the data; I.A. developed computational approaches to derive nucleosome maps from the read locations and developed the associated browser; B.F.P. directed the project, interpreted the data, and wrote the paper. S6). Those 112,750 nucleosomes detected three or more times were further analyzed, although patterns were identical when all nucleosomes were analyzed. The internal median error of the data was 4 bp (Fig. S7). H2A.Z nucleosomes were predominantly distributed at 175 bp intervals from the TSS (compared to 165 ...

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“…There is ample genetic and biochemical evidence from budding yeast, zebrafish, roundworm, fruitfly, and mammalian systems that Spt5 and Spt4 exert both negative and positive effects on transcription elongation (Hartzog et al 1998;Andrulis et al 2000;Guo et al 2000;Renner et al 2001;Shim et al 2002;Wu et al 2003;Jennings et al 2004). Spt5 is a large polypeptide (z1000-1200 amino acids) composed of multiple domain modules, including an acidic N-terminal domain, central NusG-like NGN (NusG N-terminal homology), and KOW domains (Hartzog et al 1998;Wade et al 1998a;Ponting 2002), and a CTD targeted for threonine phosphorylation Yamada et al 2006).…”

Section: Introductionmentioning

confidence: 99%

Characterization of the Schizosaccharomyces pombe Spt5-Spt4 complex

Schwer

Schneider²,

Pei³

et al. 2009

RNA

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The Spt5-Spt4 complex regulates early transcription elongation by RNA polymerase II and has an imputed role in pre-mRNA processing via its physical association with mRNA capping enzymes. Here we characterize the Schizosaccharomyces pombe core Spt5-Spt4 complex as a heterodimer and map a trypsin-resistant Spt4-binding domain within the Spt5 subunit. A genetic analysis of Spt4 in S. pombe revealed it to be inessential for growth at 25°C-30°C but critical at 37°C. These results echo the conditional spt4D growth phenotype in budding yeast, where we find that Saccharomyces cerevisiae and S. pombe Spt4 are functionally interchangeable. Complementation of S. cerevisiae spt4D and a two-hybrid assay for Spt4-Spt5 interaction provided a readout of the effects of 33 missense and truncation mutations on S. pombe Spt4 function in vivo, which were interpreted in light of the recent crystal structure of S. cerevisiae Spt4 fused to a fragment of Spt5. Our results highlight the importance of the Spt4 Zn 2+ -binding residues-Cys12, Cys15, Cys29, and Asp32-and of Ser57, a conserved constituent of the Spt4-Spt5 interface. The 990-amino acid S. pombe Spt5 protein has an exceptionally regular carboxyl-terminal domain (CTD) composed of 18 nonapeptide repeats. We find that as few as three nonamer repeats sufficed for S. pombe growth, but only when Spt4 was present. Synthetic lethality of the spt5 1-835 spt4D double mutant at 34°C suggests that interaction of Spt4 with the central domain of Spt5 overlaps functionally with the Spt5 CTD.

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NELF and DSIF cause promoter proximal pausing on thehsp70promoter inDrosophila

Cited by 279 publications

References 65 publications

Imaging Drosophila gene activation and polymerase pausing in vivo

Imaging Drosophila gene activation and polymerase pausing in vivo

Nucleosome organization in the Drosophila genome

Characterization of the Schizosaccharomyces pombe Spt5-Spt4 complex

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