Wed, 20 Aug 2008 21:21:41 BST CiteULike: massivemayhem's genome http://www.citeulike.org/user/massivemayhem/tag/genome CiteULike.org en-gb Copyright © 2004-2008 citeulike.org http://www.citeulike.org/user/massivemayhem/article/2102204 <i>Nucl. Acids Res. (12 December 2007), gkm882.</i><br /><br />KEGG (http://www.genome.jp/kegg/) is a database of biological systems that integrates genomic, chemical and systemic functional information. KEGG provides a reference knowledge base for linking genomes to life through the process of PATHWAY mapping, which is to map, for example, a genomic or transcriptomic content of genes to KEGG reference pathways to infer systemic behaviors of the cell or the organism. In addition, KEGG provides a reference knowledge base for linking genomes to the environment, such as for the analysis of drug-target relationships, through the process of BRITE mapping. KEGG BRITE is an ontology database representing functional hierarchies of various biological objects, including molecules, cells, organisms, diseases and drugs, as well as relationships among them. KEGG PATHWAY is now supplemented with a new global map of metabolic pathways, which is essentially a combined map of about 120 existing pathway maps. In addition, smaller pathway modules are defined and stored in KEGG MODULE that also contains other functional units and complexes. The KEGG resource is being expanded to suit the needs for practical applications. KEGG DRUG contains all approved drugs in the US and Japan, and KEGG DISEASE is a new database linking disease genes, pathways, drugs and diagnostic markers. 10.1093/nar/gkm882 KEGG for linking genomes to life and the environment Minoru Kanehisa Michihiro Araki Susumu Goto Masahiro Hattori Mika Hirakawa Masumi Itoh Toshiaki Katayama Shuichi Kawashima Shujiro Okuda Toshiaki Tokimatsu Yoshihiro Yamanishi doi:10.1093/nar/gkm882 Nucl. Acids Res. (12 December 2007), gkm882. 2007-12-13T06:01:37-00:00 2007 Nucl. Acids Res. gkm882 database genome pathways http://www.citeulike.org/user/massivemayhem/article/1260809 <i>Nucleic Acids Res, Vol. 35, No. Database issue. (January 2007)</i><br /><br />The Ensembl (http://www.ensembl.org/) project provides a comprehensive and integrated source of annotation of chordate genome sequences. Over the past year the number of genomes available from Ensembl has increased from 15 to 33, with the addition of sites for the mammalian genomes of elephant, rabbit, armadillo, tenrec, platypus, pig, cat, bush baby, common shrew, microbat and european hedgehog; the fish genomes of stickleback and medaka and the second example of the genomes of the sea squirt (Ciona savignyi) and the mosquito (Aedes aegypti). Some of the major features added during the year include the first complete gene sets for genomes with low-sequence coverage, the introduction of new strain variation data and the introduction of new orthology/paralog annotations based on gene trees. Ensembl 2007. TJ Hubbard BL Aken K Beal B Ballester M Caccamo Y Chen L Clarke G Coates F Cunningham T Cutts T Down SC Dyer S Fitzgerald J Fernandez-Banet S Graf S Haider M Hammond J Herrero R Holland K Howe K Howe N Johnson A Kahari D Keefe F Kokocinski E Kulesha D Lawson I Longden C Melsopp K Megy P Meidl B Ouverdin A Parker A Prlic S Rice D Rios M Schuster I Sealy J Severin G Slater D Smedley G Spudich S Trevanion A Vilella J Vogel S White M Wood T Cox V Curwen R Durbin XM Fernandez-Suarez P Flicek A Kasprzyk G Proctor S Searle J Smith A Ureta-Vidal E Birney Nucleic Acids Res, Vol. 35, No. Database issue. (January 2007) 2007-04-27T17:06:10-00:00 2007 Nucleic Acids Res 1362-4962 35 Database issue database genome sequence http://www.citeulike.org/user/massivemayhem/article/1618977 <i>PLoS Biology, Vol. 5, No. 10. (1 October 2007), e254.</i><br /><br />Presented here is a genome sequence of an individual human. It was produced from ∼32 million random DNA fragments, sequenced by Sanger dideoxy technology and assembled into 4,528 scaffolds, comprising 2,810 million bases (Mb) of contiguous sequence with approximately 7.5-fold coverage for any given region. We developed a modified version of the Celera assembler to facilitate the identification and comparison of alternate alleles within this individual diploid genome. Comparison of this genome and the National Center for Biotechnology Information human reference assembly revealed more than 4.1 million DNA variants, encompassing 12.3 Mb. These variants (of which 1,288,319 were novel) included 3,213,401 single nucleotide polymorphisms (SNPs), 53,823 block substitutions (2–206 bp), 292,102 heterozygous insertion/deletion events (indels)(1–571 bp), 559,473 homozygous indels (1–82,711 bp), 90 inversions, as well as numerous segmental duplications and copy number variation regions. Non-SNP DNA variation accounts for 22% of all events identified in the donor, however they involve 74% of all variant bases. This suggests an important role for non-SNP genetic alterations in defining the diploid genome structure. Moreover, 44% of genes were heterozygous for one or more variants. Using a novel haplotype assembly strategy, we were able to span 1.5 Gb of genome sequence in segments >200 kb, providing further precision to the diploid nature of the genome. These data depict a definitive molecular portrait of a diploid human genome that provides a starting point for future genome comparisons and enables an era of individualized genomic information. The Diploid Genome Sequence of an Individual Human Samuel Levy Granger Sutton Pauline Ng Lars Feuk Aaron Halpern Brian Walenz Nelson Axelrod Jiaqi Huang Ewen Kirkness Gennady Denisov Yuan Lin Jeffrey Macdonald Andy Pang Mary Shago Timothy Stockwell Alexia Tsiamouri Vineet Bafna Vikas Bansal Saul Kravitz Dana Busam Karen Beeson Tina Mcintosh Karin Remington Josep Abril John Gill Jon Borman Yu-Hui Rogers Marvin Frazier Stephen Scherer Robert Strausberg Craig Venter doi:10.1371/journal.pbio.0050254 PLoS Biology, Vol. 5, No. 10. (1 October 2007), e254. 2007-09-04T11:15:47-00:00 2007 PLoS Biology 5 10 e254 genome