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• W2913124539 endingPage "168" @default.
• W2913124539 startingPage "159" @default.
• W2913124539 abstract "Bipolar disorder (BD) is one of the most heritable psychiatric disorders. A growing number of whole-exome sequencing (WES) studies for BD has been performed, however, no research has examined the association between single nucleotide variants (SNVs) from WES and structural magnetic resonance imaging (MRI) data. We sequenced whole-exomes in 53 patients with BD and 82 healthy control participants at an initial discovery stage and investigated the impacts of SNVs in risk genes from WES analysis on the cortical gray-matter thickness and integrity of white matter tracts and in the following stage. Cortical thickness and white matter integrity were investigated using the FreeSurfer and TRACULA (Tracts Constrained by UnderLying Anatomy). We identified 122 BD-related genes including KMT2C, AHNAK, CDH23, DCHS1, FRAS1, MACF1 and RYR3 and observed 27 recurrent copy number alteration regions including gain on 8p23.1 and loss on 15q11.1 - q11.2. Among them, single nucleotide polymorphism (SNP) rs4639425 in KMT2C gene, which regulates histone H3 lysine 4 (H3K4) methylation involved in chromatin remodeling, was associated with widespread alterations of white matter integrity including the cingulum, uncinate fasciculus, cortico-spinal tract, and superior longitudinal fasciculus. The small sample size of patients with BD in the genome data may cause our study to be underpowered when searching for putative rare mutations. This study first combined a WES approach and neuroimaging findings in psychiatric disorders. We postulate the rs4639425 may be associated with BD-related microstructural changes of white matter tracts." @default.
• W2913124539 created "2019-02-21" @default.
• W2913124539 creator A5001289234 @default.
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• W2913124539 creator A5048836467 @default.
• W2913124539 creator A5068252846 @default.
• W2913124539 creator A5087271168 @default.
• W2913124539 date "2019-04-01" @default.
• W2913124539 modified "2023-10-13" @default.
• W2913124539 title "Whole-exome sequencing identifies variants associated with structural MRI markers in patients with bipolar disorders" @default.
• W2913124539 cites W1485272045 @default.
• W2913124539 cites W1490183063 @default.
• W2913124539 cites W1594877745 @default.
• W2913124539 cites W1858020582 @default.
• W2913124539 cites W1887013179 @default.
• W2913124539 cites W1968643437 @default.
• W2913124539 cites W1976555450 @default.
• W2913124539 cites W1984068087 @default.
• W2913124539 cites W1984168743 @default.
• W2913124539 cites W1997031801 @default.
• W2913124539 cites W2007581301 @default.
• W2913124539 cites W2008113145 @default.
• W2913124539 cites W2008197172 @default.
• W2913124539 cites W2008627757 @default.
• W2913124539 cites W2012378795 @default.
• W2913124539 cites W2013472529 @default.
• W2913124539 cites W2014509529 @default.
• W2913124539 cites W2023962370 @default.
• W2913124539 cites W2026898868 @default.
• W2913124539 cites W2032431957 @default.
• W2913124539 cites W2040420874 @default.
• W2913124539 cites W2041915741 @default.
• W2913124539 cites W2048922260 @default.
• W2913124539 cites W2049733177 @default.
• W2913124539 cites W2050161506 @default.
• W2913124539 cites W2052648508 @default.
• W2913124539 cites W2056551165 @default.
• W2913124539 cites W2058623711 @default.
• W2913124539 cites W2059145105 @default.
• W2913124539 cites W2067369841 @default.
• W2913124539 cites W2082872941 @default.
• W2913124539 cites W2086189477 @default.
• W2913124539 cites W2103441770 @default.
• W2913124539 cites W2104766386 @default.
• W2913124539 cites W2108234281 @default.
• W2913124539 cites W2108994842 @default.
• W2913124539 cites W2110579639 @default.
• W2913124539 cites W2112313406 @default.
• W2913124539 cites W2114613490 @default.
• W2913124539 cites W2124649657 @default.
• W2913124539 cites W2127442418 @default.
• W2913124539 cites W2128857247 @default.
• W2913124539 cites W2135438065 @default.
• W2913124539 cites W2141113506 @default.
• W2913124539 cites W2143359963 @default.
• W2913124539 cites W2149723686 @default.
• W2913124539 cites W2151834457 @default.
• W2913124539 cites W2160435411 @default.
• W2913124539 cites W2161633633 @default.
• W2913124539 cites W2168133698 @default.
• W2913124539 cites W2171483753 @default.
• W2913124539 cites W2269065902 @default.
• W2913124539 cites W2293668140 @default.
• W2913124539 cites W2299964679 @default.
• W2913124539 cites W2343238279 @default.
• W2913124539 cites W2364307501 @default.
• W2913124539 cites W2377806758 @default.
• W2913124539 cites W2397430163 @default.
• W2913124539 cites W2398481640 @default.
• W2913124539 cites W2412580951 @default.
• W2913124539 cites W2519531315 @default.
• W2913124539 cites W2530894206 @default.
• W2913124539 cites W2578360375 @default.
• W2913124539 cites W2587901680 @default.
• W2913124539 cites W2589115623 @default.
• W2913124539 cites W2593370030 @default.
• W2913124539 cites W2602464712 @default.
• W2913124539 cites W2606592417 @default.
• W2913124539 cites W2611569922 @default.
• W2913124539 cites W2768464064 @default.
• W2913124539 cites W2771531657 @default.
• W2913124539 cites W2792941228 @default.
• W2913124539 cites W2799558871 @default.
• W2913124539 cites W2803542287 @default.
• W2913124539 cites W2885674345 @default.
• W2913124539 cites W2889572670 @default.
• W2913124539 cites W2899514622 @default.
• W2913124539 cites W2906300019 @default.
• W2913124539 cites W3042079074 @default.
• W2913124539 cites W331238426 @default.
• W2913124539 cites W4211069648 @default.
• W2913124539 cites W4238041664 @default.
• W2913124539 doi "https://doi.org/10.1016/j.jad.2019.02.028" @default.

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