Brain proteome-wide association study implicates novel proteins in depression pathogenesis

Depression is a common condition, but current treatments are only effective in a subset of individuals. To identify new treatment targets, we integrated depression genome-wide association study (GWAS) results ( N = 500,199) with human brain proteomes ( N = 376) to perform a proteome-wide associati...

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Veröffentlicht in:	Nature neuroscience 2021-06, Vol.24 (6), p.810-817
Hauptverfasser:	Wingo, Thomas S., Liu, Yue, Gerasimov, Ekaterina S., Gockley, Jake, Logsdon, Benjamin A., Duong, Duc M., Dammer, Eric B., Lori, Adriana, Kim, Paul J., Ressler, Kerry J., Beach, Thomas G., Reiman, Eric M., Epstein, Michael P., De Jager, Philip L., Lah, James J., Bennett, David A., Seyfried, Nicholas T., Levey, Allan I., Wingo, Aliza P.
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Schlagworte:	45 631/208/199 692/699/476/1414 Animal Genetics and Genomics Behavioral Sciences Biological Techniques Biomedical and Life Sciences Biomedicine Brain Brain - pathology Brain research Databases, Genetic Depression - genetics Depression - pathology Depression, Mental Development and progression Gene expression Genes Genetic aspects Genetic Predisposition to Disease - genetics Genome-wide association studies Genome-Wide Association Study - methods Genomes Human performance Humans Mental depression Neurobiology Neurosciences Pathogenesis Protein-protein interactions Proteins Proteome - genetics Proteomes Proteomics Proteomics - methods Randomization Systematic review Target recognition
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creator	Wingo, Thomas S. Liu, Yue Gerasimov, Ekaterina S. Gockley, Jake Logsdon, Benjamin A. Duong, Duc M. Dammer, Eric B. Lori, Adriana Kim, Paul J. Ressler, Kerry J. Beach, Thomas G. Reiman, Eric M. Epstein, Michael P. De Jager, Philip L. Lah, James J. Bennett, David A. Seyfried, Nicholas T. Levey, Allan I. Wingo, Aliza P.
description	Depression is a common condition, but current treatments are only effective in a subset of individuals. To identify new treatment targets, we integrated depression genome-wide association study (GWAS) results ( N = 500,199) with human brain proteomes ( N = 376) to perform a proteome-wide association study of depression followed by Mendelian randomization. We identified 19 genes that were consistent with being causal in depression, acting via their respective cis -regulated brain protein abundance. We replicated nine of these genes using an independent depression GWAS ( N = 307,353) and another human brain proteomic dataset ( N = 152). Eleven of the 19 genes also had cis -regulated mRNA levels that were associated with depression, based on integration of the depression GWAS with human brain transcriptomes ( N = 888). Meta-analysis of the discovery and replication proteome-wide association study analyses identified 25 brain proteins consistent with being causal in depression, 20 of which were not previously implicated in depression by GWAS. Together, these findings provide promising brain protein targets for further mechanistic and therapeutic studies. Wingo et al. integrate depression GWAS results with human brain proteomes to perform proteome-wide association studies followed by Mendelian randomization. They identify 25 proteins as potential causal mediators of depression, of which 20 are new.
doi_str_mv	10.1038/s41593-021-00832-6
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To identify new treatment targets, we integrated depression genome-wide association study (GWAS) results ( N = 500,199) with human brain proteomes ( N = 376) to perform a proteome-wide association study of depression followed by Mendelian randomization. We identified 19 genes that were consistent with being causal in depression, acting via their respective cis -regulated brain protein abundance. We replicated nine of these genes using an independent depression GWAS ( N = 307,353) and another human brain proteomic dataset ( N = 152). Eleven of the 19 genes also had cis -regulated mRNA levels that were associated with depression, based on integration of the depression GWAS with human brain transcriptomes ( N = 888). Meta-analysis of the discovery and replication proteome-wide association study analyses identified 25 brain proteins consistent with being causal in depression, 20 of which were not previously implicated in depression by GWAS. 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To identify new treatment targets, we integrated depression genome-wide association study (GWAS) results ( N = 500,199) with human brain proteomes ( N = 376) to perform a proteome-wide association study of depression followed by Mendelian randomization. We identified 19 genes that were consistent with being causal in depression, acting via their respective cis -regulated brain protein abundance. We replicated nine of these genes using an independent depression GWAS ( N = 307,353) and another human brain proteomic dataset ( N = 152). Eleven of the 19 genes also had cis -regulated mRNA levels that were associated with depression, based on integration of the depression GWAS with human brain transcriptomes ( N = 888). Meta-analysis of the discovery and replication proteome-wide association study analyses identified 25 brain proteins consistent with being causal in depression, 20 of which were not previously implicated in depression by GWAS. Together, these findings provide promising brain protein targets for further mechanistic and therapeutic studies. Wingo et al. integrate depression GWAS results with human brain proteomes to perform proteome-wide association studies followed by Mendelian randomization. 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subjects	45 631/208/199 692/699/476/1414 Animal Genetics and Genomics Behavioral Sciences Biological Techniques Biomedical and Life Sciences Biomedicine Brain Brain - pathology Brain research Databases, Genetic Depression - genetics Depression - pathology Depression, Mental Development and progression Gene expression Genes Genetic aspects Genetic Predisposition to Disease - genetics Genome-wide association studies Genome-Wide Association Study - methods Genomes Human performance Humans Mental depression Neurobiology Neurosciences Pathogenesis Protein-protein interactions Proteins Proteome - genetics Proteomes Proteomics Proteomics - methods Randomization Systematic review Target recognition
title	Brain proteome-wide association study implicates novel proteins in depression pathogenesis
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