<rdf:RDF xmlns:rdf="http://www.openarchives.org/OAI/2.0/rdf/" xmlns:ow="http://www.ontoweb.org/ontology/1#" xmlns:dc="http://purl.org/dc/elements/1.1/" xmlns:ds="http://dspace.org/ds/elements/1.1/" xmlns:xsi="http://www.w3.org/2001/XMLSchema-instance" xmlns:doc="http://www.lyncode.com/xoai" xsi:schemaLocation="http://www.openarchives.org/OAI/2.0/rdf/ http://www.openarchives.org/OAI/2.0/rdf.xsd">
   <ow:Publication rdf:about="oai:digibug.ugr.es:10481/61562">
      <dc:title>Genome-wide Burden of Rare Short Deletions Is Enriched in Major Depressive Disorder in Four Cohorts</dc:title>
      <dc:creator>Zang, Xianglong</dc:creator>
      <dc:creator>Rivera Sánchez, Margarita</dc:creator>
      <dc:subject>Copy number variation</dc:subject>
      <dc:subject>Genome-wide association study (GWAS)</dc:subject>
      <dc:subject>Major depressive disorder</dc:subject>
      <dc:subject>Neuroscience</dc:subject>
      <dc:description>BACKGROUND: Major depressive disorder (MDD) is moderately heritable, with a high prevalence and a presumed&#xd;
high heterogeneity. Copy number variants (CNVs) could contribute to the heritable component of risk, but the two&#xd;
previous genome-wide association studies of rare CNVs did not report significant findings.&#xd;
METHODS: In this meta-analysis of four cohorts (5780 patients and 6626 control subjects), we analyzed the&#xd;
association of MDD to 1) genome-wide burden of rare deletions and duplications, partitioned by length (,100 kb&#xd;
or .100 kb) and other characteristics, and 2) individual rare exonic CNVs and CNV regions.&#xd;
RESULTS: Patients with MDD carried significantly more short deletions than control subjects (p = .0059) but not&#xd;
long deletions or short or long duplications. The confidence interval for long deletions overlapped with that for&#xd;
short deletions, but long deletions were 70% less frequent genome-wide, reducing the power to detect increased&#xd;
burden. The increased burden of short deletions was primarily in intergenic regions. Short deletions in cases were&#xd;
also modestly enriched for high-confidence enhancer regions. No individual CNV achieved thresholds for&#xd;
suggestive or significant association after genome-wide correction. p values , .01 were observed for 15q11.2&#xd;
duplications (TUBGCP5, CYFIP1, NIPA1, and NIPA2), deletions in or near PRKN or MSR1, and exonic&#xd;
duplications of ATG5.&#xd;
CONCLUSIONS: The increased burden of short deletions in patients with MDD suggests that rare CNVs increase the&#xd;
risk of MDD by disrupting regulatory regions. Results for longer deletions were less clear, but no large effects were&#xd;
observed for long multigenic CNVs (as seen in schizophrenia and autism). Further studies with larger sample sizes are&#xd;
warranted.</dc:description>
      <dc:date>2020-04-24T09:54:27Z</dc:date>
      <dc:date>2020-04-24T09:54:27Z</dc:date>
      <dc:date>2019</dc:date>
      <dc:type>info:eu-repo/semantics/article</dc:type>
      <dc:identifier>Zhang, X., Abdellaoui, A., Rucker, J., de Jong, S., Potash, J. B., Weissman, M. M., ... &amp; Sobell, J. (2019). Genome-wide burden of rare short deletions is enriched in major depressive disorder in four cohorts. Biological psychiatry, 85(12), 1065-1073.</dc:identifier>
      <dc:identifier>http://hdl.handle.net/10481/61562</dc:identifier>
      <dc:identifier>10.1016/j.biopsych.2019.02.022</dc:identifier>
      <dc:language>eng</dc:language>
      <dc:relation>info:eu-repo/grantAgreement/EC/FP7/115008</dc:relation>
      <dc:rights>http://creativecommons.org/licenses/by-nc-nd/3.0/es/</dc:rights>
      <dc:rights>info:eu-repo/semantics/openAccess</dc:rights>
      <dc:rights>Atribución-NoComercial-SinDerivadas 3.0 España</dc:rights>
      <dc:publisher>Elsevier Inc.</dc:publisher>
   </ow:Publication>
</rdf:RDF>