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A bivalent chromatin structure marks key developmental genes in embryonic stem cells, Cell 125

by Bradley E. Bernstein, Tarjei S. Mikkelsen, Xiaohui Xie, Michael Kamal, Dana J. Huebert, James Cuff, Ben Fry, Alex Meissner, Marius Wernig, Kathrin Plath, Rudolf Jaenisch, Re Wagschal, Robert Feil, Stuart L. Schreiber, Eric S. L , 2006
"... The most highly conserved noncoding elements (HCNEs) in mammalian genomes cluster within regions enriched for genes encoding developmentally important transcription factors (TFs). This suggests that HCNE-rich regions may contain key regulatory controls involved in development. We explored this by ex ..."
Abstract - Cited by 269 (2 self) - Add to MetaCart
this by examining histone methylation in mouse embryonic stem (ES) cells across 56 large HCNE-rich loci. We identified a specific modification pattern, termed ‘‘bivalent domains,’ ’ consisting of large regions of H3 lysine 27 methylation harboring smaller regions of H3 lysine 4 methylation. Bivalent domains tend

MicroRNA genes are transcribed by RNA polymerase II

by Yoontae Lee, Minju Kim, Jinju Han, Kyu-hyun Yeom, Sanghyuk Lee, Sung Hee Baek, V Narry Kim - EMBO J , 2004
"... MicroRNAs (miRNAs) constitute a large family of noncod-ing RNAs that function as guide molecules in diverse gene silencing pathways. Current efforts are focused on the regulatory function of miRNAs, while little is known about how these unusual genes themselves are regulated. Here we present the fir ..."
Abstract - Cited by 491 (8 self) - Add to MetaCart
of pri-miRNAs at a concentration that selectively inhibits pol II activity. Furthermore, chromatin immunoprecipitation analyses show that pol II is physically associated with a miRNA promoter. We also describe, for the first time, the detailed structure of a miRNA gene by determining the promoter

Topological domains in mammalian genomes identified by analysis of chromatin interactions. Nature 485: 376–380

by Jesse R. Dixon, Siddarth Selvaraj, Feng Yue, Audrey Kim, Yan Li, Yin Shen, Jun S. Liu, Bing Ren , 2012
"... The spatial organization of the genome is intimately linked to its biological function, yet our understanding of higher order genomic structure is coarse, fragmented and incomplete. In the nucleus of eukaryotic cells, interphase chromosomes occupy distinct chromosome territories (CT), and numerous m ..."
Abstract - Cited by 219 (4 self) - Add to MetaCart
models have been proposed for how chromosomes fold within CTs1. These models, however, provide only few mechanistic details about the relationship between higher order chromatin structure and genome function. Recent advances in genomic technologies have led to rapid revolutions in the study of 3D genome

Megabase chromatin domains involved in DNA double-strand breaks in vivo

by Emmy P. Rogakou, Chye Boon, Christophe Redon, William M. Bonner - J. Cell , 1999
"... Abstract. The loss of chromosomal integrity from DNA double-strand breaks introduced into mammalian cells by ionizing radiation results in the specific phosphorylation of histone H2AX on serine residue 139, yielding a specific modified form named �-H2AX. An antibody prepared to the unique region of ..."
Abstract - Cited by 203 (2 self) - Add to MetaCart
. The results further suggest the possible existence of units of higher order chromatin structure involved in monitoring DNA integrity. Key words: ionizing radiation • histone H2AX • DNA double-strand breaks • phosphorylation • indirect immunofluorescence THE universal presence of ionizing radiation poses a

Distinct and predictive chromatin signatures of transcriptional promoters and enhancers in the human genome.

by Nathaniel D Heintzman , Rhona K Stuart , Gary Hon , Yutao Fu , Christina W Ching , R David Hawkins , Leah O Barrera , Sara Van Calcar , Chunxu Qu , Keith A Ching , Wei Wang , Zhiping Weng , Roland D Green , Gregory E Crawford , Bing Ren - Nat. Genet., , 2007
"... Eukaryotic gene transcription is accompanied by acetylation and methylation of nucleosomes near promoters, but the locations and roles of histone modifications elsewhere in the genome remain unclear. We determined the chromatin modification states in high resolution along 30 Mb of the human genome ..."
Abstract - Cited by 202 (3 self) - Add to MetaCart
and cofactors on regulatory DNA sequences such as promoters and enhancers and on the chromatin structure containing these elements 1-3 . Promoters are located at the 5¢ ends of genes immediately surrounding the transcriptional start site (TSS) and serve as the point of assembly of the transcriptional machinery

Genomewide analysis of PRC1 and PRC2 occupancy identifies two classes of bivalent domains

by Manching Ku, Richard P. Koche, Esther Rheinbay, Eric M. Mendenhall, Endoh Tarjei S. Mikkelsen, Bradley E. Bernstein - PLoS Genet , 2008
"... In embryonic stem (ES) cells, bivalent chromatin domains with overlapping repressive (H3 lysine 27 tri-methylation) and activating (H3 lysine 4 tri-methylation) histonemodifications mark the promoters of more than 2,000 genes. To gain insight into the structure and function of bivalent domains, we m ..."
Abstract - Cited by 74 (2 self) - Add to MetaCart
In embryonic stem (ES) cells, bivalent chromatin domains with overlapping repressive (H3 lysine 27 tri-methylation) and activating (H3 lysine 4 tri-methylation) histonemodifications mark the promoters of more than 2,000 genes. To gain insight into the structure and function of bivalent domains, we

A probabilistic functional network of yeast genes

by Insuk Lee, Shailesh V. Date, Alex T. Adai, Edward M. Marcotte - Science , 2004
"... A conceptual framework for integrating diverse functional genomics data was developed by reinterpreting experiments to provide numerical likelihoods that genes are functionally linked. This allows direct comparison and integration of different classes of data. The resulting probabilistic gene networ ..."
Abstract - Cited by 207 (13 self) - Add to MetaCart
-scale interaction assays. The integrated linkages distinguish true from false-positive interactions in earlier data sets; new interactions emerge from genes ’ network contexts, as shown for genes in chromatin modification and ribosome biogenesis. Knowledge of the correct overall structures of gene networks

chromatin

by Alexey A. Gavrilov, Ekaterina S. Gushchanskaya, Olga Strelkova, Oksana Zhironkina, Igor I. Kireev, Olga V. Iarovaia, Sergey V. Razin , 2012
"... Disclosure of a structural milieu for the proximity ligation reveals the elusive nature of an active ..."
Abstract - Add to MetaCart
Disclosure of a structural milieu for the proximity ligation reveals the elusive nature of an active

Genetic and functional diversification of small RNA pathways in plants

by Zhixin Xie, Lisa K. Johansen, Adam M. Gustafson, Kristin D. Kasschau, Andrew D. Lellis, Daniel Zilberman, Steven E. Jacobsen, James C. Carrington - PLoS Biol , 2004
"... Multicellular eukaryotes produce small RNA molecules (approximately 21–24 nucleotides) of two general types, microRNA (miRNA) and short interfering RNA (siRNA). They collectively function as sequence-specific guides to silence or regulate genes, transposons, and viruses and to modify chromatin and g ..."
Abstract - Cited by 185 (17 self) - Add to MetaCart
and diversification of DCL and RDR genes during evolution of plants contributed to specialization of small RNA-directed pathways for development, chromatin structure, and defense.

Stage-Specific Germ-Cell Marker Genes Are Expressed in All Mouse Pluripotent Cell Types and Emerge Early during Induced Pluripotency

by Xingbo Xu, D. V. Krishna Pantakani, Ra Lührig, Xiaoying Tan, Tatjana Khromov, Jessica Nolte, Ralf Dressel, Ulrich Zechner, Wolfgang Engel , 2011
"... Embryonic stem cells (ESCs) generated from the in-vitro culture of blastocyst stage embryos are known as equivalent to blastocyst inner cell mass (ICM) in-vivo. Though several reports have shown the expression of germ cell/pre-meiotic (GC/ PrM) markers in ESCs, their functional relevance for the plu ..."
Abstract - Cited by 5 (2 self) - Add to MetaCart
. Further, siRNA knockdown experiments have demonstrated the parallel maintenance and independence of pluripotent and GC/PrM networks in ESCs. Through chromatin immunoprecipitation experiments, we observed that pluripotent cells exhibit active chromatin states at GC marker genes and a bivalent chromatin
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