Journal Article10.1038/NG1637
Genome-scale profiling of histone H3.3 replacement patterns.
TL;DR: It is proposed that deposition and inheritance of actively modified H3.3 in regulatory regions maintains transcriptionally active chromatin and is introduced a new strategy for profiling epigenetic patterns on the basis of H 3.3 replacement.
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Abstract: Histones of multicellular organisms are assembled into chromatin primarily during DNA replication. When chromatin assembly occurs at other times, the histone H3.3 variant replaces canonical H3. Here we introduce a new strategy for profiling epigenetic patterns on the basis of H3.3 replacement, using microarrays covering roughly one-third of the Drosophila melanogaster genome at 100-bp resolution. We identified patterns of H3.3 replacement over active genes and transposons. H3.3 replacement occurred prominently at sites of abundant RNA polymerase II and methylated H3 Lys4 throughout the genome and was enhanced on the dosage-compensated male X chromosome. Active genes were depleted of histones at promoters and were enriched in H3.3 from upstream to downstream of transcription units. We propose that deposition and inheritance of actively modified H3.3 in regulatory regions maintains transcriptionally active chromatin.
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Citations
Histone variants at a glance.
Paul B. Talbert,Steven Henikoff +1 more
TL;DR: In this paper, the authors briefly examine new insights into histone origins and discuss variants from each of the histone families, focusing on how structural differences may alter their functions, including DNA repair, chromosome segregation and regulation of transcription initiation.
Epigenetics in Insects: Genome Regulation and the Generation of Phenotypic Diversity.
TL;DR: This review provides an introduction to the field of molecular epigenetics in insects and provides a brief overview of techniques for profiling and perturbing individual facets of the epigenome.
144
Drosophila MSL complex globally acetylates H4K16 on the male X chromosome for dosage compensation
Marnie E. Gelbart,Erica Larschan,Erica Larschan,Shouyong Peng,Shouyong Peng,Shouyong Peng,Peter J. Park,Peter J. Park,Mitzi I. Kuroda,Mitzi I. Kuroda +9 more
TL;DR: Almost all active genes on the X chromosome are associated with robust H4 Lys16 acetylation (H4K16ac), the histone modification catalyzed by the MSL complex, suggesting a common principle for the establishment of active and silenced chromatin domains.
143
High expression of the mammalian X chromosome in brain
TL;DR: The exceptionally important role of the X chromosome in brain function, evident from the prevalence of X-linked forms of mental retardation, is discussed in view of sex chromosome regulation and evolution and sexual reproduction.
141
Genome-wide mapping and analysis of active promoters in mouse embryonic stem cells and adult organs
Leah O. Barrera,Zirong Li,Andrew D. Smith,Karen C. Arden,Webster K. Cavenee,Michael Q. Zhang,Roland Green,Bing Ren +7 more
TL;DR: Promoters with enriched activity in mouse embryonic stem cells as well as adult brain, heart, kidney, and liver are characterized, showing that promoters with CpG islands are typically non-tissue specific and that a subset appear to be persistently marked by active chromatin modifications in the absence of detectable Polr2a binding.
References
Genomic Maps and Comparative Analysis of Histone Modifications in Human and Mouse
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TL;DR: Methylation patterns at orthologous loci are strongly conserved between human and mouse even though many methylated sites do not show sequence conservation notably higher than background, which suggests that the DNA elements that direct the methylation represent only a small fraction of the region or lie at some distance from the site.
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Genome-wide analysis of DNA copy-number changes using cDNA microarrays.
Jonathan R. Pollack,Charles M. Perou,Ash A. Alizadeh,Michael B. Eisen,Alexander Pergamenschikov,Cheryl F. Williams,Stefanie S. Jeffrey,David Botstein,Patrick O. Brown,Patrick O. Brown +9 more
TL;DR: This work describes a cDNA microarray-based CGH method, and its application to DNA copy-number variation analysis in breast cancer cell lines and tumours, and identifies gene amplifications and deletions genome-wide and with high resolution.
Histone H3.1 and H3.3 Complexes Mediate Nucleosome Assembly Pathways Dependent or Independent of DNA Synthesis
TL;DR: Deposition of the major histone H3 (H3.1) is coupled to DNA synthesis during DNA replication and possibly DNA repair, whereas histone variant H3.3 serves as the replacement variant for the DNA-synthesis-independent deposition pathway, and purified deposition machineries for these histones are presented.
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Genome-scale identification of nucleosome positions in S. cerevisiae.
Guo-Cheng Yuan,Yuen-Jong Liu,Michael F. Dion,Michael D. Slack,Lani F. Wu,Steven J. Altschuler,Oliver J. Rando +6 more
TL;DR: The authors used a tiled microarray approach to identify at high resolution the translational positions of 2278 nucleosomes over 482 kilobases of Saccharomyces cerevisiae DNA.
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Epigenetic Regulation of Cellular Memory by the Polycomb and Trithorax Group Proteins
Leonie Ringrose,Renato Paro +1 more
TL;DR: Current ideas on the protein and DNA components of this transcriptional memory system are reviewed and how they interact dynamically with each other to orchestrate cellular memory for several hundred genes are reviewed.
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