SREBP Controls Oxygen-Dependent Mobilization of Retrotransposons in Fission Yeast

Sehgal, Alfica; Lee, Chih-Yung S.; Espenshade, Peter J.

doi:10.1371/journal.pgen.0030131.eor

Cited by 17 publications

(27 citation statements)

References 39 publications

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“…As Abp1 and Cbh1 can bind to distinct loci, and that these factors do not always colocalize with SHREC 23 , CENP-B binding in contexts other than heterochromatin and transposable elements might recruit activities important for other chromatin transactions, such as transcription and DNA replication. Accumulating evidence implicates transposable-element-derived sequences as regulators of gene expression in diverse species 1, [35][36][37] . A substantial fraction of human promoters contains transposable element sequences 38 , and instances of their contribution to gene regulation have been documented 1, 39 .…”

Section: Discussionmentioning

confidence: 99%

Host genome surveillance for retrotransposons by transposon-derived proteins

Cam¹,

Noma²,

Ebina

et al. 2007

Nature

161

241

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Transposable elements and their remnants constitute a substantial fraction of eukaryotic genomes. Host genomes have evolved defence mechanisms, including chromatin modifications and RNA interference, to regulate transposable elements. Here we describe a genome surveillance mechanism for retrotransposons by transposase-derived centromeric protein CENP-B homologues of the fission yeast Schizosaccharomyces pombe. CENP-B homologues of S. pombe localize at and recruit histone deacetylases to silence Tf2 retrotransposons. CENP-Bs also repress solo long terminal repeats (LTRs) and LTR-associated genes. Tf2 elements are clustered into 'Tf' bodies, the organization of which depends on CENP-Bs that display discrete nuclear structures. Furthermore, CENP-Bs prevent an 'extinct' Tf1 retrotransposon from re-entering the host genome by blocking its recombination with extant Tf2, and silence and immobilize a Tf1 integrant that becomes sequestered into Tf bodies. Our results reveal a probable ancient retrotransposon surveillance pathway important for host genome integrity, and highlight potential conflicts between DNA transposons and retrotransposons, major transposable elements believed to have greatly moulded the evolution of genomes.

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Section: Discussionmentioning

confidence: 99%

Host genome surveillance for retrotransposons by transposon-derived proteins

Cam¹,

Noma²,

Ebina

et al. 2007

Nature

161

241

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“…5F). Tf2 mobilization is often mediated by integrase-independent recombination between its cDNA and pre-existing genomic copies of Tf2 (Hoff et al 1998;Sehgal et al 2007). We speculate that the binding of Rad52 to an immature form of Tf2 cDNA may contribute to this main mode of Tf2 transposition.…”

Section: Rad52 Enrichment Patterns In Pfh1 Helicase Mutantsmentioning

confidence: 96%

“…To verify the SPI-seq results, we performed ChIP-PCR analysis using strains in which one Tf2 is tagged with a neo marker (Sehgal et al 2007). Indeed, in D1D3, we detected Rad52 enrichment on the neo marker gene (Fig.…”

Section: Rad52 Enrichment Patterns In Pfh1 Helicase Mutantsmentioning

confidence: 99%

Mapping genomic hotspots of DNA damage by a single-strand-DNA-compatible and strand-specific ChIP-seq method

Zhou

Zhang

et al. 2012

Genome Res.

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Spontaneous DNA damage may occur nonrandomly in the genome, especially when genome maintenance mechanisms are undermined. We developed single-strand DNA (ssDNA)-associated protein immunoprecipitation followed by sequencing (SPI-seq) to map genomic hotspots of DNA damage. We demonstrated this method with Rad52, a homologous recombination repair protein, which binds to ssDNA formed at DNA lesions. SPI-seq faithfully detected, in fission yeast, Rad52 enrichment at artificially induced double-strand breaks (DSBs) as well as endogenously programmed DSBs for mating-type switching. Applying Rad52 SPI-seq to fission yeast mutants defective in DNA helicase Pfh1 or histone H3K56 deacetylase Hst4, led to global views of DNA lesion hotspots emerging in these mutants. We also found serendipitously that histone dosage aberration can activate retrotransposon Tf2 and cause the accumulation of a Tf2 cDNA species bound by Rad52. SPI-seq should be widely applicable for mapping sites of DNA damage and uncovering the causes of genome instability.

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“…1B). The reporter gene consisted of four tandem Sre1N DNA-binding sites driving expression of ura4 ϩ that codes for orotidine 5-monophosphate decarboxylase and is required for growth in the absence of uracil (18,36). Orotidine 5-monophosphate decarboxylase also enables the cells to metabolize the compound 5-FOA to the toxin 5-fluorouracil; thus, cells that highly express ura4 ϩ fail to grow in the presence of 5-FOA (29).…”

Section: Identification Of Sre1nmentioning

confidence: 99%

Casein Kinase 1 Regulates Sterol Regulatory Element-binding Protein (SREBP) to Control Sterol Homeostasis

Brookheart

Lee

Espenshade

2014

Journal of Biological Chemistry

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Background: SREBP transcription factor controls sterol homeostasis. Results: Fission yeast casein kinase 1 (CK1) binds and accelerates degradation of active SREBP, inhibiting expression of target genes and decreasing ergosterol. Conclusion: CK1 controls nuclear SREBP stability to regulate sterol homeostasis in fission yeast. Significance: CK1 is the first kinase shown to regulate fungal SREBP and functions in the control of SREBP and sterol homeostasis.

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SREBP Controls Oxygen-Dependent Mobilization of Retrotransposons in Fission Yeast

Cited by 17 publications

References 39 publications

Host genome surveillance for retrotransposons by transposon-derived proteins

Host genome surveillance for retrotransposons by transposon-derived proteins

Mapping genomic hotspots of DNA damage by a single-strand-DNA-compatible and strand-specific ChIP-seq method

Casein Kinase 1 Regulates Sterol Regulatory Element-binding Protein (SREBP) to Control Sterol Homeostasis

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