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Photoswitched DNA-Binding of a Photochromic Spiropyran
pubs.acs.org
Posted by laffieya to DNA on Thu Sep 04 2008 at 00:54 UTC | info | related
 
Generation of High Density Protein Microarrays by Cell-free in Situ Expression of Unpurified PCR Products
Philipp Angenendt et al.
Molecular Cellular Proteomics 5 (9), 1658-66 (01 Sep 2006)
 
DNA
www.nature.com
Posted by Baloghca to DNA on Wed Sep 03 2008 at 18:49 UTC | info | related
 
PLoS Genetics: Double Strand Breaks Can Initiate Gene Silencing and SIRT1-Dependent Onset of DNA Methylation in an Exogenous Promoter CpG Island
www.plosgenetics.org
Chronic exposure to inducers of DNA base oxidation and single and double strand breaks contribute to tumorigenesis. In addition to the genetic changes caused by this DNA damage, such tumors often contain epigenetically silenced genes with aberrant promoter region CpG island DNA hypermethylation. We herein explore the relationships between such DNA damage and epigenetic gene silencing using an experimental model in which we induce a defined double strand break in an exogenous promoter construct of the E-cadherin CpG island, which is frequently aberrantly DNA hypermethylated in epithelial cancers. Following the onset of repair of the break, we observe recruitment to the site of damage of key proteins involved in establishing and maintaining transcriptional repression, namely SIRT1, EZH2, DNMT1, and DNMT3B, and the appearance of the silencing histone modifications, hypoacetyl H4K16, H3K9me2 and me3, and H3K27me3. Although in most cells selected after the break, DNA repair occurs faithfully with preservation of activity of the promoter, a small percentage of the plated cells demonstrate induction of heritable silencing. The chromatin around the break site in such a silent clone is enriched for most of the above silent chromatin proteins and histone marks, and the region harbors the appearance of increasing DNA methylation in the CpG island of the promoter. During the acute break, SIRT1 appears to be required for the transient recruitment of DNMT3B and subsequent methylation of the promoter in the silent clones. Taken together, our data suggest that normal repair of a DNA break can occasionally cause heritable silencing of a CpG island–containing promoter by recruitment of proteins involved in silencing. Furthermore, with contribution of the stress-related protein SIRT1, the break can lead to the onset of aberrant CpG island DNA methylation, which is frequently associated with tight gene silencing in cancer.
Posted by taniusha and 1 other with 1 comment to methylation DNA on Mon Sep 01 2008 at 08:15 UTC | info | related
 
Microbulbifer celer sp. nov., isolated from a marine solar saltern of the Yellow Sea in Korea
Jung-Hoon Yoon et al.
International journal of systematic and evolutionary microbiology 57 (Pt 10), 2365-9 (Oct 2007)
 
Enzymatic properties and nucleotide and amino acid sequences of a thermostable beta-agarase from a novel species of deep-sea Microbulbifer
Y Ohta et al.
Applied microbiology and biotechnology 64 (4), 505-14 (May 2004)
 
Microbulbifer hydrolyticus gen. nov., sp. nov., and Marinobacterium georgiense gen. nov., sp. nov., two marine bacteria from a lignin-rich pulp mill waste enrichment community
J M González et al.
International journal of systematic bacteriology 47 (2), 369-76 (Apr 1997)
 
Sensitive mutation detection in heterogeneous cancer specimens by massively parallel picoliter reactor sequencing
Nature Medicine 12 (7), 852-5 (Jul 2006)
 
DNA repair progress
Nanomedicinecenter.com, (27 Aug 2008)
Nice progress
Posted by mistic to nanomedicine Repair DNA on Wed Aug 27 2008 at 12:44 UTC | info | related
 
Recognition of Guanine Structure in Nucleic Acids by Nickel Complexes
Accounts of Chemical Research 27 (10), 295 (1994)

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