Preferential Genome Targeting of the CBP Co-Activator by Rel and Smad Proteins in Early Drosophila melanogaster Embryos

Holmqvist, Per-Henrik; Boija, Ann; Philip, Philge; Crona, Filip; Stenberg, Per; Mannervik, Mattias

doi:10.1371/journal.pgen.1002769

Cited by 42 publications

(57 citation statements)

References 45 publications

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“…The following antibodies were used for histone modifications: H3 (Abcam, ab1791); H3K4me3 (Millipore, 07-473); H3K9me3 (Abcam, ab8898); H3K18ac (Abcam, ab1191); H3K27ac (Abcam, ab4729); H3K27me3 (Abcam, ab6002); basal transcription machinery, Rpb3 (gift from John Lis, Cornell University, Ithaca, NY); 8WG16 (Abcam, ab817); PolII S5 (Abcam, ab5131); TBP (Robert Tjian, University of California, Berkeley); transcription factor, Dorsal (Christos Samakovlis, Stockholm University, Stockholm); and chromatin regulators, CBP (described in ref. 24) and Polycomb (Yuri Schwartz, Umeå University, Umeå, Sweden).…”

Section: Methodsmentioning

confidence: 99%

“…Dorsal and the CBP/p300 coactivator (nejire) preferentially co-occupy genomic DNA genomewide, genetically interact, and bind each other in vitro and in vivo (23,24). Interestingly, ChIP of the CBP coactivator showed high occupancy of the brk and sog enhancers in the neuroectoderm, but only occupancy at background levels in the mesoderm (P < 0.05, Fig.…”

Section: Consistent With This Idea Studies Inmentioning

confidence: 97%

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Initiation of diverse epigenetic states during nuclear programming of the Drosophila body plan

Boija

Mannervik

2016

Proc. Natl. Acad. Sci. U.S.A.

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Epigenetic patterns of histone modifications contribute to the maintenance of tissue-specific gene expression. Here, we show that such modifications also accompany the specification of cell identities by the NF-κB transcription factor Dorsal in the precellular Drosophila embryo. We provide evidence that the maternal pioneer factor, Zelda, is responsible for establishing poised RNA polymerase at Dorsal target genes before Dorsal-mediated zygotic activation. At the onset of cell specification, Dorsal recruits the CBP/p300 coactivator to the regulatory regions of defined target genes in the presumptive neuroectoderm, resulting in their histone acetylation and transcriptional activation. These genes are inactive in the mesoderm due to transcriptional quenching by the Snail repressor, which precludes recruitment of CBP and prevents histone acetylation. By contrast, inactivation of the same enhancers in the dorsal ectoderm is associated with Polycomb-repressed H3K27me3 chromatin. Thus, the Dorsal morphogen gradient produces three distinct histone signatures including two modes of transcriptional repression, active repression (hypoacetylation), and inactivity (H3K27me3). Whereas histone hypoacetylation is associated with a poised polymerase, H3K27me3 displaces polymerase from chromatin. Our results link different modes of RNA polymerase regulation to separate epigenetic patterns and demonstrate that developmental determinants orchestrate differential chromatin states, providing new insights into the link between epigenetics and developmental patterning.eneration of many specialized cell types from an identical DNA sequence is a remarkable property of genomes in multicellular organisms. Cell fate is specified by transcription factors through the initiation of differential gene expression patterns, but maintenance of cell-type-specific gene expression programs often relies on epigenetic mechanisms (reviewd in ref. 1). Epigenetic events such as Polycomb-mediated repression are therefore important for maintenance of specific cell identities and have been implicated in human disease (reviewed in refs. 2 and 3), but how differences in epigenetic information between cell types arise is poorly understood.The repressive nature of chromatin limits access of proteins to DNA. Pioneer factors facilitate chromatin opening, allowing additional proteins to bind DNA (reviewed in ref. 4). In the Drosophila embryo, zygotic genome activation occurs with the help of Zelda (5), a transcription factor with many features of a pioneer factor. Zelda associates with target genes before their activation (6, 7) and increases chromatin accessibility (8-11). Zelda facilitates DNA binding of other transcription factors, including Dorsal, a Rel-family transcription factor related to mammalian NF-κB (9).Formation of the three germ layers, mesoderm, neuroectoderm, and dorsal ectoderm, in Drosophila embryos involves establishment of differential gene expression patterns by the Dorsal morphogen (reviewed in refs. 12 and 13) (Fig. 1A). Dorsal forms an intr...

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Section: Methodsmentioning

confidence: 99%

Section: Consistent With This Idea Studies Inmentioning

confidence: 97%

Initiation of diverse epigenetic states during nuclear programming of the Drosophila body plan

Boija

Mannervik

2016

Proc. Natl. Acad. Sci. U.S.A.

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“…In gastrulation defective (gd) mutant embryos gd 7 , Dl is not activated, resulting in uniformly high signaling activity of the fly BMP2/4 ortholog Decapentaplegic (Dpp) but below wildtype maximum levels (see Ashe and Levine 1999) and the specification of dorsal ectodermal fate in the entire embryo. These mutants have frequently been used in the past because they allow the analysis of patterning across the Dl activity gradient (e.g., Stathopoulos et al 2002;Zeitlinger et al 2007;Holmqvist et al 2012) and have helped DV patterning become one of the beststudied gene regulatory networks in development. The DV patterning system also illustrates another important principle of pattern formation, the widespread use and requirement of sequence-specific transcriptional repressors.…”

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confidence: 99%

Drosophilapoised enhancers are generated during tissue patterning with the help of repression

Koenecke

Johnston

et al. 2016

Genome Res.

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Histone modifications are frequently used as markers for enhancer states, but how to interpret enhancer states in the context of embryonic development is not clear. The poised enhancer signature, involving H3K4me1 and low levels of H3K27ac, has been reported to mark inactive enhancers that are poised for future activation. However, future activation is not always observed, and alternative reasons for the widespread occurrence of this enhancer signature have not been investigated. By analyzing enhancers during dorsal-ventral (DV) axis formation in the Drosophila embryo, we find that the poised enhancer signature is specifically generated during patterning in the tissue where the enhancers are not induced, including at enhancers that are known to be repressed by a transcriptional repressor. These results suggest that, rather than serving exclusively as an intermediate step before future activation, the poised enhancer state may be a mark for spatial regulation during tissue patterning. We discuss the possibility that the poised enhancer state is more generally the result of repression by transcriptional repressors.

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“…A, CBP and Bicoid occupancy at the gt locus in WT embryos. ChIP-sequencing peaks for CBP (73) and ChIP-chip peaks for Bicoid (82) in 2-4-h old WT embryos are shown for the gt locus. Occupancy is plotted as log 2 -fold enrichment over input.…”

Section: Core Promoter-preferential Activation Of Ftz Is Mediated Viamentioning

confidence: 99%

Structure-Function Analysis of the Drosophila melanogaster Caudal Transcription Factor Provides Insights into Core Promoter-preferential Activation

Shir-Shapira

Sharabany

Filderman

et al. 2015

Journal of Biological Chemistry

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Background: Caudal is a core promoter-preferential transcription factor. Results: We defined functional regions in Caudal that are important for core promoter-preferential activation and demonstrated that dCBP confers core promoter-preferential activation. Conclusion:The unique combination of Caudal and dCBP enables co-activation in a core promoter-preferential manner. Significance: We provide mechanistic insights into core promoter-enhancer compatibility.

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Preferential Genome Targeting of the CBP Co-Activator by Rel and Smad Proteins in Early Drosophila melanogaster Embryos

Cited by 42 publications

References 45 publications

Initiation of diverse epigenetic states during nuclear programming of the Drosophila body plan

Initiation of diverse epigenetic states during nuclear programming of the Drosophila body plan

Drosophilapoised enhancers are generated during tissue patterning with the help of repression

Structure-Function Analysis of the Drosophila melanogaster Caudal Transcription Factor Provides Insights into Core Promoter-preferential Activation

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