Literature DB >> 16223876

Comparative gene expression analysis of blood and brain provides concurrent validation of SELENBP1 up-regulation in schizophrenia.

Stephen J Glatt1, Ian P Everall, William S Kremen, Jacques Corbeil, Roman Sásik, Negar Khanlou, Mark Han, Choong-Chin Liew, Ming T Tsuang.   

Abstract

Microarray techniques hold great promise for identifying risk factors for schizophrenia (SZ) but have not yet generated widely reproducible results due to methodological differences between studies and the high risk of type I inferential errors. Here we established a protocol for conservative analysis and interpretation of gene expression data from the dorsolateral prefrontal cortex of SZ patients using statistical and bioinformatic methods that limit false positives. We also compared brain gene expression profiles with those from peripheral blood cells of a separate sample of SZ patients to identify disease-associated genes that generalize across tissues and populations and further substantiate the use of gene expression profiling of blood for detecting valid SZ biomarkers. Implementing this systematic approach, we: (i) discovered 177 putative SZ risk genes in brain, 28 of which map to linked chromosomal loci; (ii) delineated six biological processes and 12 molecular functions that may be particularly disrupted in the illness; (iii) identified 123 putative SZ biomarkers in blood, 6 of which (BTG1, GSK3A, HLA-DRB1, HNRPA3, SELENBP1, and SFRS1) had corresponding differential expression in brain; (iv) verified the differential expression of the strongest candidate SZ biomarker (SELENBP1) in blood; and (v) demonstrated neuronal and glial expression of SELENBP1 protein in brain. The continued application of this approach in other brain regions and populations should facilitate the discovery of highly reliable and reproducible candidate risk genes and biomarkers for SZ. The identification of valid peripheral biomarkers for SZ may ultimately facilitate early identification, intervention, and prevention efforts as well.

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Year:  2005        PMID: 16223876      PMCID: PMC1266138          DOI: 10.1073/pnas.0507666102

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  28 in total

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Journal:  Mol Psychiatry       Date:  2004-07       Impact factor: 15.992

8.  Low blood selenium concentrations in schizophrenic patients on clozapine.

Authors:  K S Vaddadi; E Soosai; G Vaddadi
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Journal:  Genome Biol       Date:  2003-03-25       Impact factor: 13.583

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Journal:  Am J Hum Genet       Date:  2003-06-11       Impact factor: 11.025

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  129 in total

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3.  Exon expression and alternatively spliced genes in Tourette Syndrome.

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Review 4.  Convergent Functional Genomics of bipolar disorder: from animal model pharmacogenomics to human genetics and biomarkers.

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7.  TP53 Polymorphism Contributes to the Susceptibility to Bipolar Disorder but Not to Schizophrenia in the Chinese Han Population.

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Journal:  J Mol Neurosci       Date:  2019-05-05       Impact factor: 3.444

8.  Gene expression before HAART initiation predicts HIV-infected individuals at risk of poor CD4+ T-cell recovery.

Authors:  Christopher H Woelk; Nadejda Beliakova-Bethell; Miguel Goicoechea; Yingdong Zhao; Pinyi Du; Steffney E Rought; Jean Lozach; Josué Pérez-Santiago; Douglas D Richman; Davey M Smith; Susan J Little
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9.  Pharmacogenomic predictors of citalopram treatment outcome in major depressive disorder.

Authors:  Firoza Mamdani; Marcelo T Berlim; Marie-Martine Beaulieu; Gustavo Turecki
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10.  Transcriptomic analysis of postmortem brain identifies dysregulated splicing events in novel candidate genes for schizophrenia.

Authors:  Ori S Cohen; Sarah Y Mccoy; Frank A Middleton; Sean Bialosuknia; Yanli Zhang-James; Lu Liu; Ming T Tsuang; Stephen V Faraone; Stephen J Glatt
Journal:  Schizophr Res       Date:  2012-10-09       Impact factor: 4.939

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