Post-mortem molecular profiling of three psychiatric disorders

Ryne C. Ramaker; Kevin M. Bowling; Brittany N. Lasseigne; Megan Hastings Hagenauer; Andrew A. Hardigan; Nicholas S. Davis; Jason Gertz; Preston Cartagena; David Walsh; Marquis P. Vawter; Edward G. Jones; Alan F. Schatzberg; Jack D. Barchas; Stanley J. Watson; Blynn G. Bunney; Huda Akil; William E. Bunney; Jun Z. Li; Sara J. Cooper; R Myers

doi:10.1186/s13073-017-0458-5

Post-mortem molecular profiling of three psychiatric disorders

Ryne C. Ramaker(University of Alabama at Birmingham), Kevin M. Bowling(HudsonAlpha Institute for Biotechnology), Brittany N. Lasseigne(HudsonAlpha Institute for Biotechnology), Megan Hastings Hagenauer(University of Michigan–Ann Arbor), Andrew A. Hardigan(HudsonAlpha Institute for Biotechnology), Nicholas S. Davis(HudsonAlpha Institute for Biotechnology), Jason Gertz(University of Utah), Preston Cartagena(University of California, Irvine), David Walsh(University of California, Irvine), Marquis P. Vawter(University of California, Irvine), Edward G. Jones(HudsonAlpha Institute for Biotechnology), Alan F. Schatzberg(Stanford University), Jack D. Barchas(Cornell University), Stanley J. Watson(University of Michigan–Ann Arbor), Blynn G. Bunney(University of California, Irvine), Huda Akil(University of Michigan–Ann Arbor), William E. Bunney(University of California, Irvine), Jun Z. Li(University of Michigan–Ann Arbor), Sara J. Cooper(HudsonAlpha Institute for Biotechnology), R Myers(HudsonAlpha Institute for Biotechnology)

Genome Medicine

July 28, 2017

10.1186/s13073-017-0458-5

Cited by 212Open Access

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Abstract

BACKGROUND: Psychiatric disorders are multigenic diseases with complex etiology that contribute significantly to human morbidity and mortality. Although clinically distinct, several disorders share many symptoms, suggesting common underlying molecular changes exist that may implicate important regulators of pathogenesis and provide new therapeutic targets. METHODS: We performed RNA sequencing on tissue from the anterior cingulate cortex, dorsolateral prefrontal cortex, and nucleus accumbens from three groups of 24 patients each diagnosed with schizophrenia, bipolar disorder, or major depressive disorder, and from 24 control subjects. We identified differentially expressed genes and validated the results in an independent cohort. Anterior cingulate cortex samples were also subjected to metabolomic analysis. ChIP-seq data were used to characterize binding of the transcription factor EGR1. RESULTS: We compared molecular signatures across the three brain regions and disorders in the transcriptomes of post-mortem human brain samples. The most significant disease-related differences were in the anterior cingulate cortex of schizophrenia samples compared to controls. Transcriptional changes were assessed in an independent cohort, revealing the transcription factor EGR1 as significantly down-regulated in both cohorts and as a potential regulator of broader transcription changes observed in schizophrenia patients. Additionally, broad down-regulation of genes specific to neurons and concordant up-regulation of genes specific to astrocytes was observed in schizophrenia and bipolar disorder patients relative to controls. Metabolomic profiling identified disruption of GABA levels in schizophrenia patients. CONCLUSIONS: We provide a comprehensive post-mortem transcriptome profile of three psychiatric disorders across three brain regions. We highlight a high-confidence set of independently validated genes differentially expressed between schizophrenia and control patients in the anterior cingulate cortex and integrate transcriptional changes with untargeted metabolite profiling.

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