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authorBonface2024-02-09 09:41:28 -0600
committerMunyoki Kilyungi2024-08-09 13:30:43 +0300
commitd029d5d7f8ead1f1de8d318045004a4a6f68f5fb (patch)
tree33c7ff40e3f953d030ed08f468f7afb1dfcba9e6 /general/datasets/OXUKHS_ILMLiver_RI0510
parent769ff7825f5d8d36d541e90534c07f1985899973 (diff)
downloadgn-docs-d029d5d7f8ead1f1de8d318045004a4a6f68f5fb.tar.gz
Update dataset RTF Files.
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-rw-r--r--general/datasets/OXUKHS_ILMLiver_RI0510/platform.rtf1
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+<p>HS Northport stock (see&nbsp;https://www.nature.com/articles/ng1840) descended from&nbsp;eight inbred progenitor strains (A/J, AKR/J, BALBc/J, CBA/J, C3H/HeJ, C57BL/6J, DBA/2J and LP/J). For details, please see&nbsp;Demarest, K., Koyner, J., McCaughran, J. Jr., Cipp, L. &amp; Hitzemann, R.&nbsp;<cite>Further characterization and high-resolution mapping of quantitative trait loci for ethanol-induced locomotor activity</cite>.&nbsp;<i>Behav. Genet.</i>31, 79&ndash;91 (2001).</p>
diff --git a/general/datasets/OXUKHS_ILMLiver_RI0510/platform.rtf b/general/datasets/OXUKHS_ILMLiver_RI0510/platform.rtf
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+<p>Organism: Mus musculus. Tissue: Liver. Array design: A-MEXP-533 - Illumina Mouse-6 v1 Expression BeadChip</p>
diff --git a/general/datasets/OXUKHS_ILMLiver_RI0510/summary.rtf b/general/datasets/OXUKHS_ILMLiver_RI0510/summary.rtf
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+<p>A proportion of the genetic variants underlying complex phenotypes do so through their effects on gene expression, so an important challenge in complex trait analysis is to discover the genetic basis for the variation in transcript abundance. So far, the potential of mapping both quantitative trait loci (QTLs) and expression quantitative trait loci (eQTLs) in rodents has been limited by the low mapping resolution inherent in crosses between inbred strains. We provide a megabase resolution map of thousands of eQTLs in hippocampus, lung, and liver samples from heterogeneous stock (HS) mice in which 843 QTLs have also been mapped at megabase resolution. We exploit dense mouse SNP data to show that artifacts due to allele-specific hybridization occur in _30% of the cis-acting eQTLs and, by comparison with exon expression data, we show that alternative splicing of the 3_ end of the genes accounts for &lt;1% of cis-acting eQTLs. Approximately one third of cis-acting eQTLs and one half of trans-acting eQTLs are tissue specific. We have created an important systems biology resource for the genetic analysis of complex traits in a key model organism.</p>