Critical Appraisal of DNA Microarrays in Psychiatric Genomics

Transcriptome profiling using DNA microarrays are data-driven approaches with the potential to uncover unanticipated relationships between gene expression alterations and psychiatric disorders. Studies to date have yielded both convergent and divergent findings. Differences may be explained, at leas...

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Published inBiological psychiatry (1969) Vol. 60; no. 2; pp. 163 - 176
Main Authors Mirnics, Károly, Levitt, Pat, Lewis, David A.
Format Journal Article
LanguageEnglish
Published New York, NY Elsevier Inc 15.07.2006
Elsevier Science
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Abstract Transcriptome profiling using DNA microarrays are data-driven approaches with the potential to uncover unanticipated relationships between gene expression alterations and psychiatric disorders. Studies to date have yielded both convergent and divergent findings. Differences may be explained, at least in part, by the use of a variety of microarray platforms and analytical approaches. Consistent findings across studies suggest, however, that important relationships may exist between altered gene expression and genetic susceptibility to psychiatric disorders. For example, GAD67, RGS4, DTNBP1, NRG1, and GABRAB2 show expression alterations in the postmortem brain of subjects with schizophrenia, and these genes have been also implicated as putative, heritable schizophrenia susceptibility genes. Thus, we propose that for some genes, altered expression in the postmortem human brain may have a dual origin: polymorphisms in the candidate genes themselves or upstream genetic–environmental factors that converge to alter their expression level. We hypothesize that certain gene products, which function as “molecular hubs,” commonly show altered expression in psychiatric disorders and confer genetic susceptibility for one or more diseases. Microarray gene expression studies are ideally suited to reveal these putative disease-associated molecular hubs and to identify promising candidates for genetic association studies.
AbstractList Transcriptome profiling using DNA microarrays are data-driven approaches with the potential to uncover unanticipated relationships between gene expression alterations and psychiatric disorders. Studies to date have yielded both convergent and divergent findings. Differences may be explained, at least in part, by the use of a variety of microarray platforms and analytical approaches. Consistent findings across studies suggest, however, that important relationships may exist between altered gene expression and genetic susceptibility to psychiatric disorders. For example, GAD67, RGS4, DTNBP1, NRG1, and GABRAB2 show expression alterations in the postmortem brain of subjects with schizophrenia, and these genes have been also implicated as putative, heritable schizophrenia susceptibility genes. Thus, we propose that for some genes, altered expression in the postmortem human brain may have a dual origin: polymorphisms in the candidate genes themselves or upstream genetic–environmental factors that converge to alter their expression level. We hypothesize that certain gene products, which function as “molecular hubs,” commonly show altered expression in psychiatric disorders and confer genetic susceptibility for one or more diseases. Microarray gene expression studies are ideally suited to reveal these putative disease-associated molecular hubs and to identify promising candidates for genetic association studies.
Transcriptome profiling using DNA microarrays are data-driven approaches with the potential to uncover unanticipated relationships between gene expression alterations and psychiatric disorders. Studies to date have yielded both convergent and divergent findings. Differences may be explained, at least in part, by the use of a variety of microarray platforms and analytical approaches. Consistent findings across studies suggest, however, that important relationships may exist between altered gene expression and genetic susceptibility to psychiatric disorders. For example, GAD67, RGS4, DTNBP1, NRG1, and GABRAB2 show expression alterations in the postmortem brain of subjects with schizophrenia, and these genes have been also implicated as putative, heritable schizophrenia susceptibility genes. Thus, we propose that for some genes, altered expression in the postmortem human brain may have a dual origin: polymorphisms in the candidate genes themselves or upstream genetic-environmental factors that converge to alter their expression level. We hypothesize that certain gene products, which function as "molecular hubs," commonly show altered expression in psychiatric disorders and confer genetic susceptibility for one or more diseases. Microarray gene expression studies are ideally suited to reveal these putative disease-associated molecular hubs and to identify promising candidates for genetic association studies.Transcriptome profiling using DNA microarrays are data-driven approaches with the potential to uncover unanticipated relationships between gene expression alterations and psychiatric disorders. Studies to date have yielded both convergent and divergent findings. Differences may be explained, at least in part, by the use of a variety of microarray platforms and analytical approaches. Consistent findings across studies suggest, however, that important relationships may exist between altered gene expression and genetic susceptibility to psychiatric disorders. For example, GAD67, RGS4, DTNBP1, NRG1, and GABRAB2 show expression alterations in the postmortem brain of subjects with schizophrenia, and these genes have been also implicated as putative, heritable schizophrenia susceptibility genes. Thus, we propose that for some genes, altered expression in the postmortem human brain may have a dual origin: polymorphisms in the candidate genes themselves or upstream genetic-environmental factors that converge to alter their expression level. We hypothesize that certain gene products, which function as "molecular hubs," commonly show altered expression in psychiatric disorders and confer genetic susceptibility for one or more diseases. Microarray gene expression studies are ideally suited to reveal these putative disease-associated molecular hubs and to identify promising candidates for genetic association studies.
Author Mirnics, Károly
Levitt, Pat
Lewis, David A.
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  surname: Mirnics
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– sequence: 2
  givenname: Pat
  surname: Levitt
  fullname: Levitt, Pat
  organization: Department of Psychiatry, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania
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  surname: Lewis
  fullname: Lewis, David A.
  organization: Department of Psychiatry, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania
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IsPeerReviewed true
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Issue 2
Keywords DNA microarray
human brain
transcriptome
gene expression
psychiatric disorders
Human
Central nervous system
DNA chip
Mental disorder
Gene expression
Encephalon
Language English
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Snippet Transcriptome profiling using DNA microarrays are data-driven approaches with the potential to uncover unanticipated relationships between gene expression...
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SubjectTerms Adult and adolescent clinical studies
Biological and medical sciences
DNA - genetics
DNA microarray
gene expression
Gene Expression Regulation - genetics
Gene Expression Regulation - physiology
Genomics - instrumentation
human brain
Humans
Medical sciences
Mental Disorders - genetics
Miscellaneous
Oligonucleotide Array Sequence Analysis
psychiatric disorders
Psychiatry - instrumentation
Psychology. Psychoanalysis. Psychiatry
Psychopathology. Psychiatry
transcriptome
Title Critical Appraisal of DNA Microarrays in Psychiatric Genomics
URI https://www.clinicalkey.com/#!/content/1-s2.0-S000632230600134X
https://dx.doi.org/10.1016/j.biopsych.2006.02.003
https://www.ncbi.nlm.nih.gov/pubmed/16616896
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