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Systems genetics identifies a convergent gene network for cognition and neurodevelopmental disease

Systems genetics identifies a convergent gene network for cognition and neurodevelopmental disease
Systems genetics identifies a convergent gene network for cognition and neurodevelopmental disease
Genetic determinants of cognition are poorly characterized, and their relationship to genes that confer risk for neurodevelopmental disease is unclear. Here we performed a systems-level analysis of genome-wide gene expression data to infer gene-regulatory networks conserved across species and brain regions. Two of these networks, M1 and M3, showed replicable enrichment for common genetic variants underlying healthy human cognitive abilities, including memory. Using exome sequence data from 6,871 trios, we found that M3 genes were also enriched for mutations ascertained from patients with neurodevelopmental disease generally, and intellectual disability and epileptic encephalopathy in particular. M3 consists of 150 genes whose expression is tightly developmentally regulated, but which are collectively poorly annotated for known functional pathways. These results illustrate how systems-level analyses can reveal previously unappreciated relationships between neurodevelopmental disease–associated genes in the developed human brain, and provide empirical support for a convergent gene-regulatory network influencing cognition and neurodevelopmental disease.
1097-6256
223-232
Johnson, Michael R
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Shkura, Kirill
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Langley, Sarah R
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Delahaye-duriez, Andree
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Srivastava, Prashant
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Hill, W David
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Rackham, Owen J L
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Davies, Gail
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Harris, Sarah E
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Moreno-Moral, Aida
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Rotival, Maxime
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Speed, Doug
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Petrovski, Slavé
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Katz, Anaïs
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Hayward, Caroline
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Smith, Blair H
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Padmanabhan, Sandosh
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Hocking, Lynne J
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Starr, John M
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Liewald, David C
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Visconti, Alessia
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Falchi, Mario
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Bottolo, Leonardo
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Rossetti, Tiziana
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Danis, Bénédicte
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Mazzuferi, Manuela
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Foerch, Patrik
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Grote, Alexander
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Helmstaedter, Christoph
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Becker, Albert J
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Kaminski, Rafal M
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Deary, Ian J
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Petretto, Enrico
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Johnson, Michael R
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Shkura, Kirill
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Langley, Sarah R
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Hill, W David
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Speed, Doug
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Hayward, Caroline
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Porteous, David J
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Smith, Blair H
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Padmanabhan, Sandosh
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Hocking, Lynne J
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Starr, John M
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Foerch, Patrik
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Grote, Alexander
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Helmstaedter, Christoph
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Becker, Albert J
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Kaminski, Rafal M
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Deary, Ian J
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Petretto, Enrico
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Johnson, Michael R, Shkura, Kirill, Langley, Sarah R, Delahaye-duriez, Andree, Srivastava, Prashant, Hill, W David, Rackham, Owen J L, Davies, Gail, Harris, Sarah E, Moreno-Moral, Aida, Rotival, Maxime, Speed, Doug, Petrovski, Slavé, Katz, Anaïs, Hayward, Caroline, Porteous, David J, Smith, Blair H, Padmanabhan, Sandosh, Hocking, Lynne J, Starr, John M, Liewald, David C, Visconti, Alessia, Falchi, Mario, Bottolo, Leonardo, Rossetti, Tiziana, Danis, Bénédicte, Mazzuferi, Manuela, Foerch, Patrik, Grote, Alexander, Helmstaedter, Christoph, Becker, Albert J, Kaminski, Rafal M, Deary, Ian J and Petretto, Enrico (2016) Systems genetics identifies a convergent gene network for cognition and neurodevelopmental disease. Nature Neuroscience, 19 (2), 223-232. (doi:10.1038/nn.4205).

Record type: Article

Abstract

Genetic determinants of cognition are poorly characterized, and their relationship to genes that confer risk for neurodevelopmental disease is unclear. Here we performed a systems-level analysis of genome-wide gene expression data to infer gene-regulatory networks conserved across species and brain regions. Two of these networks, M1 and M3, showed replicable enrichment for common genetic variants underlying healthy human cognitive abilities, including memory. Using exome sequence data from 6,871 trios, we found that M3 genes were also enriched for mutations ascertained from patients with neurodevelopmental disease generally, and intellectual disability and epileptic encephalopathy in particular. M3 consists of 150 genes whose expression is tightly developmentally regulated, but which are collectively poorly annotated for known functional pathways. These results illustrate how systems-level analyses can reveal previously unappreciated relationships between neurodevelopmental disease–associated genes in the developed human brain, and provide empirical support for a convergent gene-regulatory network influencing cognition and neurodevelopmental disease.

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More information

Accepted/In Press date: 13 November 2015
e-pub ahead of print date: 21 December 2015
Published date: 1 February 2016

Identifiers

Local EPrints ID: 444239
URI: http://eprints.soton.ac.uk/id/eprint/444239
ISSN: 1097-6256
PURE UUID: eadacdb3-f2c3-41d4-8724-f9350a0ffa2b
ORCID for Owen J L Rackham: ORCID iD orcid.org/0000-0002-4390-0872

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Date deposited: 02 Oct 2020 16:30
Last modified: 17 Mar 2024 04:03

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Contributors

Author: Michael R Johnson
Author: Kirill Shkura
Author: Sarah R Langley
Author: Andree Delahaye-duriez
Author: Prashant Srivastava
Author: W David Hill
Author: Gail Davies
Author: Sarah E Harris
Author: Aida Moreno-Moral
Author: Maxime Rotival
Author: Doug Speed
Author: Slavé Petrovski
Author: Anaïs Katz
Author: Caroline Hayward
Author: David J Porteous
Author: Blair H Smith
Author: Sandosh Padmanabhan
Author: Lynne J Hocking
Author: John M Starr
Author: David C Liewald
Author: Alessia Visconti
Author: Mario Falchi
Author: Leonardo Bottolo
Author: Tiziana Rossetti
Author: Bénédicte Danis
Author: Manuela Mazzuferi
Author: Patrik Foerch
Author: Alexander Grote
Author: Christoph Helmstaedter
Author: Albert J Becker
Author: Rafal M Kaminski
Author: Ian J Deary
Author: Enrico Petretto

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