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      Genome-wide association study in a rat model of temperament identifies multiple loci for exploratory locomotion and anxiety-like traits

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          Abstract

          Common genetic factors likely contribute to multiple psychiatric diseases including mood and substance use disorders. Certain stable, heritable traits reflecting temperament, termed externalizing or internalizing, play a large role in modulating vulnerability to these disorders. To model these heritable tendencies, we selectively bred rats for high and low exploration in a novel environment [bred High Responders (bHR) vs. Low Responders (bLR)]. To identify genes underlying the response to selection, we phenotyped and genotyped 538 rats from an F 2 cross between bHR and bLR. Several behavioral traits show high heritability, including the selection trait: exploratory locomotion (EL) in a novel environment. There were significant phenotypic and genetic correlations between tests that capture facets of EL and anxiety. There were also correlations with Pavlovian conditioned approach (PavCA) behavior despite the lower heritability of that trait. Ten significant and conditionally independent loci for six behavioral traits were identified. Five of the six traits reflect different facets of EL that were captured by three behavioral tests. Distance traveled measures from the open field and the elevated plus maze map onto different loci, thus may represent different aspects of novelty-induced locomotor activity. The sixth behavioral trait, number of fecal boli, is the only anxiety-related trait mapping to a significant locus on chromosome 18 within which the Pik3c3 gene is located. There were no significant loci for PavCA. We identified a missense variant in the Plekhf1 gene on the chromosome 1:95 Mb QTL and Fancf and Gas2 as potential candidate genes that may drive the chromosome 1:107 Mb QTL for EL traits. The identification of a locomotor activity-related QTL on chromosome 7 encompassing the Pkhd1l1 and Trhr genes is consistent with our previous finding of these genes being differentially expressed in the hippocampus of bHR vs. bLR rats. The strong heritability coupled with identification of several loci associated with exploratory locomotion and emotionality provide compelling support for this selectively bred rat model in discovering relatively large effect causal variants tied to elements of internalizing and externalizing behaviors inherent to psychiatric and substance use disorders.

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          A program for annotating and predicting the effects of single nucleotide polymorphisms, SnpEff: SNPs in the genome of Drosophila melanogaster strain w1118; iso-2; iso-3.

          Pablo E. Cingolani, Adrian E. Platts, Le Lily Wang (2012)
          We describe a new computer program, SnpEff, for rapidly categorizing the effects of variants in genome sequences. Once a genome is sequenced, SnpEff annotates variants based on their genomic locations and predicts coding effects. Annotated genomic locations include intronic, untranslated region, upstream, downstream, splice site, or intergenic regions. Coding effects such as synonymous or non-synonymous amino acid replacement, start codon gains or losses, stop codon gains or losses, or frame shifts can be predicted. Here the use of SnpEff is illustrated by annotating ~356,660 candidate SNPs in ~117 Mb unique sequences, representing a substitution rate of ~1/305 nucleotides, between the Drosophila melanogaster w(1118); iso-2; iso-3 strain and the reference y(1); cn(1) bw(1) sp(1) strain. We show that ~15,842 SNPs are synonymous and ~4,467 SNPs are non-synonymous (N/S ~0.28). The remaining SNPs are in other categories, such as stop codon gains (38 SNPs), stop codon losses (8 SNPs), and start codon gains (297 SNPs) in the 5'UTR. We found, as expected, that the SNP frequency is proportional to the recombination frequency (i.e., highest in the middle of chromosome arms). We also found that start-gain or stop-lost SNPs in Drosophila melanogaster often result in additions of N-terminal or C-terminal amino acids that are conserved in other Drosophila species. It appears that the 5' and 3' UTRs are reservoirs for genetic variations that changes the termini of proteins during evolution of the Drosophila genus. As genome sequencing is becoming inexpensive and routine, SnpEff enables rapid analyses of whole-genome sequencing data to be performed by an individual laboratory.
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            GCTA: a tool for genome-wide complex trait analysis.

            Jian Yang, S. Lee, Michael E Goddard (2011)
            For most human complex diseases and traits, SNPs identified by genome-wide association studies (GWAS) explain only a small fraction of the heritability. Here we report a user-friendly software tool called genome-wide complex trait analysis (GCTA), which was developed based on a method we recently developed to address the "missing heritability" problem. GCTA estimates the variance explained by all the SNPs on a chromosome or on the whole genome for a complex trait rather than testing the association of any particular SNP to the trait. We introduce GCTA's five main functions: data management, estimation of the genetic relationships from SNPs, mixed linear model analysis of variance explained by the SNPs, estimation of the linkage disequilibrium structure, and GWAS simulation. We focus on the function of estimating the variance explained by all the SNPs on the X chromosome and testing the hypotheses of dosage compensation. The GCTA software is a versatile tool to estimate and partition complex trait variation with large GWAS data sets.
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              Genome-wide meta-analysis of depression identifies 102 independent variants and highlights the importance of the prefrontal brain regions

              David M. Howard, Mark J. Adams, Toni‐Kim Clarke (2019)
              Major depression is a debilitating psychiatric illness that is typically associated with low mood and anhedonia. Depression has a heritable component that has remained difficult to elucidate with current sample sizes due to the polygenic nature of the disorder. To maximize sample size, we meta-analyzed data on 807,553 individuals (246,363 cases and 561,190 controls) from the three largest genome-wide association studies of depression. We identified 102 independent variants, 269 genes, and 15 genesets associated with depression, including both genes and gene pathways associated with synaptic structure and neurotransmission. An enrichment analysis provided further evidence of the importance of prefrontal brain regions. In an independent replication sample of 1,306,354 individuals (414,055 cases and 892,299 controls), 87 of the 102 associated variants were significant after multiple testing correction. These findings advance our understanding of the complex genetic architecture of depression and provide several future avenues for understanding etiology and developing new treatment approaches.
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                Author and article information

                Contributors
                Journal
                Journal ID (nlm-ta): Front Genet
                Journal ID (iso-abbrev): Front Genet
                Journal ID (publisher-id): Front. Genet.
                Title: Frontiers in Genetics
                Publisher: Frontiers Media S.A.
                ISSN (Electronic): 1664-8021
                Publication date (Electronic): 11 January 2023
                Publication date Collection: 2022
                Volume: 13
                Electronic Location Identifier: 1003074
                Affiliations
                [1] 1 Department of Psychiatry , University of California San Diego , La Jolla, CA, United States
                [2] 2 Michigan Neuroscience Institute , University of Michigan , Ann Arbor, MI, United States
                [3] 3 Department of Human Genetics , University of Michigan , Ann Arbor, MI, United States
                [4] 4 Institute for Genomic Medicine , University of California San Diego , La Jolla, CA, United States
                Author notes

                Edited by: Huiping Zhang, Boston University, United States

                Reviewed by: Daniel Gatti, Jackson Laboratory, United States

                Megan K. Mulligan, University of Tennessee Health Science Center (UTHSC), United States

                *Correspondence: Abraham A. Palmer, aap@ 123456ucsd.edu

                These authors have contributed equally to this work and share first authorship

                These authors have contributed equally to this work and share last authorship

                This article was submitted to Behavioral and Psychiatric Genetics, a section of the journal Frontiers in Genetics

                Article
                Publisher ID: 1003074
                DOI: 10.3389/fgene.2022.1003074
                PMC ID: 9873817
                PubMed ID: 36712851
                SO-VID: 1ac99caa-b944-4311-a33b-bd7344d13c22
                Copyright © Copyright © 2023 Chitre, Hebda-Bauer, Blandino, Bimschleger, Nguyen, Maras, Li, Ozel, Pan, Polesskaya, Cheng, Flagel, Watson, Li, Akil and Palmer.
                License:

                This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.

                History
                Date received : 25 July 2022
                Date accepted : 20 October 2022
                Funding
                Funded by: National Institute on Drug Abuse , doi 10.13039/100000026;
                NIDA U01DA043098 (HA, JL, AP): Office of Naval Research (ONR) 00014-19-1-2149 (HA); The Hope for Depression Research Foundation (HDRF) (HA); the Pritzker Neuropsychiatric Research Consortium (HA, SW).
                Categories
                Subject: Genetics
                Subject: Original Research

                ScienceOpen disciplines: Genetics
                Keywords: gwas,genome-wide association study,behavior,rat model,anxiety like behaviors,exploratory locomotion
                Data availability:
                ScienceOpen disciplines: Genetics
                Keywords: gwas, genome-wide association study, behavior, rat model, anxiety like behaviors, exploratory locomotion

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