Clinical exome sequencing in early-onset generalized dystonia and large-scale resequencing follow-up

Michael Zech; Sylvia Boesch; Angela Jochim; Sandrina Weber; Tobias Meindl; Barbara Schormair; Thomas Wieland; Christian Lunetta; Valeria Sansone; Michael Messner; Joerg Mueller; Andres Ceballos-Baumann; Tim M Strom; Roberto Colombo; Werner Poewe; Bernhard Haslinger; Juliane Winkelmann

doi:10.1002/mds.26808

Clinical exome sequencing in early-onset generalized dystonia and large-scale resequencing follow-up

Mov Disord. 2017 Apr;32(4):549-559. doi: 10.1002/mds.26808. Epub 2016 Sep 26.

Authors

Michael Zech^{1

2}, Sylvia Boesch³, Angela Jochim², Sandrina Weber¹, Tobias Meindl², Barbara Schormair¹, Thomas Wieland⁴, Christian Lunetta⁵, Valeria Sansone^{6

7}, Michael Messner⁸, Joerg Mueller^{3

9}, Andres Ceballos-Baumann^{2

8}, Tim M Strom^{4

10}, Roberto Colombo^{11

12}, Werner Poewe³, Bernhard Haslinger², Juliane Winkelmann^{1

2

13

14}

Affiliations

¹ Institut für Neurogenomik, Helmholtz Zentrum München, Munich, Germany.
² Klinik und Poliklinik für Neurologie, Klinikum rechts der lsar, Technische Universität München, Munich, Germany.
³ Department of Neurology, Medical University Innsbruck, Innsbruck, Austria.
⁴ Institut für Humangenetik, Helmholtz Zentrum München, Munich, Germany.
⁵ Neuromuscular Omnicentre Sud (NEMO SUD), Fondazione Aurora Onlus, Messina, Italy.
⁶ Neuromuscular Omnicentre (NEMO), Fondazione Serena Onlus, Milan, Italy.
⁷ Department of Biochemical Sciences for Health, University of Milan, Milan, Italy.
⁸ Schön Klinik München Schwabing, Munich, Germany.
⁹ Vivantes Klinikum Spandau, Berlin, Germany.
¹⁰ Institut für Humangenetik, Technische Universität München, Munich, Germany.
¹¹ Institute of Clinical Biochemistry, Catholic University, Rome, Italy.
¹² Center for the Study of Rare Hereditary Diseases, Niguarda Ca' Granda Metropolitan Hospital, Milan, Italy.
¹³ Munich Cluster for Systems Neurology, SyNergy, Munich, Germany.
¹⁴ Institute of Human Genetics, Klinikum rechts der Isar, Technical University Munich, Munich, Germany.

PMID: 27666935
DOI: 10.1002/mds.26808

Abstract

Background: Dystonia is clinically and genetically heterogeneous. Despite being a first-line testing tool for heterogeneous inherited disorders, whole-exome sequencing has not yet been evaluated in dystonia diagnostics. We set up a pilot study to address the yield of whole-exome sequencing for early-onset generalized dystonia, a disease subtype enriched for monogenic causation.

Methods: Clinical whole-exome sequencing coupled with bioinformatics analysis and detailed phenotyping of mutation carriers was performed on 16 consecutive cases with genetically undefined early-onset generalized dystonia. Candidate pathogenic variants were validated and tested for cosegregation. The whole-exome approach was complemented by analyzing 2 mutated yet unestablished causative genes in another 590 dystonia cases.

Results: Whole-exome sequencing detected clinically relevant mutations of known dystonia-related genes in 6 generalized dystonia cases (37.5%), among whom 3 had novel variants. Reflecting locus heterogeneity, identified unique variants were distributed over 5 genes (GCH1, THAP1, TOR1A, ANO3, ADCY5), of which only 1 (ANO3) was mutated recurrently. Three genes (GCH1, THAP1, TOR1A) were associated with isolated generalized dystonia, whereas 2 (ANO3, ADCY5) gave rise to combined dystonia-myoclonus phenotypes. Follow-up screening of ANO3 and ADCY5 revealed a set of distinct variants of interest, the pathogenicity of which was supported by bioinformatics testing and cosegregation work.

Conclusions: Our study identified whole-exome sequencing as an effective strategy for molecular diagnosis of early-onset generalized dystonia and offers insights into the heterogeneous genetic architecture of this condition. Furthermore, it provides confirmatory evidence for a dystonia-relevant role of ANO3 and ADCY5, both of which likely associate with a broader spectrum of dystonic expressions than previously thought. © 2016 International Parkinson and Movement Disorder Society.

Keywords: ADCY5; ANO3; diagnostics; dystonia; exome.

MeSH terms

Adenylyl Cyclases / genetics
Adult
Anoctamins
Apoptosis Regulatory Proteins / genetics
Chloride Channels / genetics
DNA Mutational Analysis
DNA-Binding Proteins / genetics
Dystonia / genetics*
Exome / genetics*
Family Health
Female
Follow-Up Studies
GTP Cyclohydrolase / genetics
Humans
Male
Middle Aged
Models, Molecular
Molecular Chaperones / genetics
Mutation / genetics*
Nuclear Proteins / genetics
Young Adult

Substances

ANO3 protein, human
Anoctamins
Apoptosis Regulatory Proteins
Chloride Channels
DNA-Binding Proteins
Molecular Chaperones
Nuclear Proteins
THAP1 protein, human
TOR1A protein, human
GTP Cyclohydrolase
Adenylyl Cyclases
adenylyl cyclase type V