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In Silico Detection of Sequence Variations Modifying Transcriptional Regulation
Malin Andersen et al.
PLoS Computational Biology 4 (1), e5 (01 Jan 2008)
Jacob Odeberg (Royal Institute of Technology, Sweden):Here we present an in silico driven approach to identify possible genetic variation in regulatory sequences. The approach combines phylogenetic footprinting and transcription factor binding site prediction to identify variation in candidate cis-regulatory elements. The bioinformatics approach has been tested on a set of SNPs that are reported to have a regulatory function, as well as background SNPs. The bioinformatics software generated for the analysis has been implemented as a Web-based application system entitled RAVEN (regulatory analysis of variation in enhancers). The RAVEN system is available at http://www.cisreg.ca
Posted by qyuan and 6 others to resource expression on Fri Jan 25 2008 at 21:42 UTC | info | related
 
Genes and (Common) Pathways Underlying Drug Addiction
Chuan-Yun Li, Xizeng Mao, and Liping Wei
PLoS Computational Biology 4 (1), e2 (01 Jan 2008)
Liping Wei (Peking University):We integrated 2,343 items of evidence from peer-reviewed publications between 1976 and 2006 linking genes and chromosome regions to addiction by single-gene strategies, microrray, proteomics, or genetic studies. We identified 1,500 human addiction-related genes and developed KARG (http://karg.cbi.pku.edu.cn), the first molecular database for addiction-related genes with extensive annotations and a friendly Web interface. We then performed a meta-analysis of 396 genes that were supported by two or more independent items of evidence to identify 18 molecular pathways that were statistically significantly enriched, covering both upstream signaling events and downstream effects. Five molecular pathways significantly enriched for all four different types of addictive drugs were identified as common pathways which may underlie shared rewarding and addictive actions, including two new ones, GnRH signaling pathway and gap junction. We connected the common pathways into a hypothetical common molecular network for addiction. We observed that fast and slow positive feedback loops were interlinked through CAMKII, which may provide clues to explain some of the irreversible features of addiction.
Posted by qyuan and 4 others to resource diseases on Fri Jan 25 2008 at 21:36 UTC | info | related
 
Complex trait analysis of gene expression uncovers polygenic and pleiotropic networks that modulate nervous system function
Elissa Chesler et al.
Nature genetics. 37 (3), 233-42 (Mar 2005)
Robert Williams (University of Tennessee Health Science Center): We profiled gene expression using Affymetrix oligonucleotide arrays in the BXD recombinant inbred strains, for which we have extensive SNP and haplotype data. We found that a small number of major-effect quantitative trait loci jointly modulated large sets of transcripts and classical neural phenotypes in patterns specific to each tissue. WebQTL: http://www.webqtl.org/
Posted by qyuan and 3 others to resource expression on Thu Jan 03 2008 at 14:17 UTC | info | related

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