Dystonia genes functionally converge in specific neurons and share neurobiology with psychiatric disorders

Author:

Mencacci Niccolò E1,Reynolds Regina H2ORCID,Ruiz Sonia Garcia2,Vandrovcova Jana3,Forabosco Paola4,Sánchez-Ferrer Alvaro56,Volpato Viola7,Botía Juan A,D'Sa Karishma,Forabosco Paola,Guelfi Sebastian,Hardy John,Vandrovcova Jana,Mackenzie Chris-Ann,Ramasamy Adaikalavan,Ryten Mina,Smith Colin,Trabzuni Daniah,Weale Michael E,Noyce Alastair J,Kaiyrzhanov Rauan,Middlehurst Ben,Kia Demis A,Tan Manuela,Houlden Henry,Morris Huw R,Plun-Favreau Helene,Holmans Peter,Hardy John,Trabzuni Daniah,Bras Jose,Quinn John,Mok Kin Y,Kinghorn Kerri J,Billingsley Kimberley,Wood Nicholas W,Lewis Patrick,Guerreiro Rita,Lovering Ruth,R’Bibo Lea,Manzoni Claudia,Rizig Mie,Ryten Mina,Guelfi Sebastian,Escott-Price Valentina,Chelban Viorica,Foltynie Thomas,Williams Nigel,Shashakin Chingiz,Zharkinbekova Nazira,Zholdybayeva Elena,Aitkulova Akbota,Harvey Kirsten,Weale Michael E8,Bhatia Kailash P9,Webber Caleb7,Hardy John231011,Botía Juan A312,Ryten Mina281314, ,

Affiliation:

1. Department of Neurology, Northwestern University Feinberg School of Medicine, Chicago, IL, 60611, USA

2. Department of Neurodegenerative Disease, Institute of Neurology, University College London, London, UK

3. Reta Lila Weston Research Laboratories, Institute of Neurology, University College London, London, UK

4. Istituto di Ricerca Genetica e Biomedica, Cittadella Universitaria di Cagliari, 09042, Monserrato, Sardinia, Italy

5. Department of Biochemistry and Molecular Biology-A, Faculty of Biology, Regional Campus of International Excellence ‘Campus Mare Nostrum’, University of Murcia, Campus Espinardo, E-30100, Murcia, Spain

6. Murcia Biomedical Research Institute (IMIB-Arrixaca), 30120, Murcia, Spain

7. UK Dementia Research Institute at Cardiff University, Hadyn Ellis Building, Cardiff, CF24 4HQ, UK

8. Department of Medical and Molecular Genetics, King's College London, Guy's Hospital, London, UK

9. Department of Clinical and Movement Neurosciences, Institute of Neurology, University College London, London, UK

10. UK Dementia Research Institute at University College London, London, UK

11. Institute for Advanced Study, The Hong Kong University of Science and Technology, Hong Kong SAR, China

12. Department of Information and Communications Engineering, University of Murcia, Spain

13. NIHR Great Ormond Street Hospital Biomedical Research Centre, University College London, London, UK

14. Genetics and Genomic Medicine, Great Ormond Street Institute of Child Health, University College London, London WC1E 6BT, UK

Abstract

Abstract Dystonia is a neurological disorder characterized by sustained or intermittent muscle contractions causing abnormal movements and postures, often occurring in absence of any structural brain abnormality. Psychiatric comorbidities, including anxiety, depression, obsessive-compulsive disorder and schizophrenia, are frequent in patients with dystonia. While mutations in a fast-growing number of genes have been linked to Mendelian forms of dystonia, the cellular, anatomical, and molecular basis remains unknown for most genetic forms of dystonia, as does its genetic and biological relationship to neuropsychiatric disorders. Here we applied an unbiased systems-biology approach to explore the cellular specificity of all currently known dystonia-associated genes, predict their functional relationships, and test whether dystonia and neuropsychiatric disorders share a genetic relationship. To determine the cellular specificity of dystonia-associated genes in the brain, single-nuclear transcriptomic data derived from mouse brain was used together with expression-weighted cell-type enrichment. To identify functional relationships among dystonia-associated genes, we determined the enrichment of these genes in co-expression networks constructed from 10 human brain regions. Stratified linkage-disequilibrium score regression was used to test whether co-expression modules enriched for dystonia-associated genes significantly contribute to the heritability of anxiety, major depressive disorder, obsessive-compulsive disorder, schizophrenia, and Parkinson’s disease. Dystonia-associated genes were significantly enriched in adult nigral dopaminergic neurons and striatal medium spiny neurons. Furthermore, 4 of 220 gene co-expression modules tested were significantly enriched for the dystonia-associated genes. The identified modules were derived from the substantia nigra, putamen, frontal cortex, and white matter, and were all significantly enriched for genes associated with synaptic function. Finally, we demonstrate significant enrichments of the heritability of major depressive disorder, obsessive-compulsive disorder and schizophrenia within the putamen, frontal cortex and white matter modules, and nominal enrichment of the heritability of Parkinson’s disease within the substantia nigra module. In conclusion, multiple dystonia-associated genes interact and contribute to pathogenesis likely through dysregulation of synaptic signalling in striatal medium spiny neurons, adult nigral dopaminergic neurons and frontal cortical neurons. Furthermore, the enrichment of the heritability of psychiatric disorders in the co-expression modules enriched for dystonia-associated genes indicates that psychiatric symptoms associated with dystonia are likely to be intrinsic to its pathophysiology.

Funder

Parkinson’s

Spanish grant ‘Ayudas a los Grupos y Unidades de Excelencia Científica de la Región de Murcia’

Fundación Séneca-Agencia de Ciencia y Tecnología de la Región de Murcia

Programa de Apoyo a la Investigación 2014

UK Dementia Research Institute

UK Medical Research Council

Alzheimer’s Society

Alzheimer’s Research UK

Tenure-track Clinician Scientist Fellowship

Publisher

Oxford University Press (OUP)

Subject

Neurology (clinical)

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