Clinical Exome Sequencing in Early-Onset Generalized Dystonia and Large-Scale Resequencing Follow-up

被引:82
|
作者
Zech, Michael [1 ,2 ]
Boesch, Sylvia [3 ]
Jochim, Angela [2 ]
Weber, Sandrina [1 ]
Meindl, Tobias [2 ]
Schormair, Barbara [1 ]
Wieland, Thomas [4 ]
Lunetta, Christian [5 ]
Sansone, Valeria [6 ,7 ]
Messner, Michael [8 ]
Mueller, Joerg [3 ,9 ]
Ceballos-Baumann, Andres [2 ,8 ]
Strom, Tim M. [4 ,10 ]
Colombo, Roberto [11 ,12 ]
Poewe, Werner [3 ]
Haslinger, Bernhard [2 ]
Winkelmann, Juliane [1 ,2 ,13 ,14 ]
机构
[1] Helmholtz Zentrum Munchen, Inst Neurogen, Munich, Germany
[2] Tech Univ Munich, Klin & Poliklin Neurol, Klinikum Rechts Isar, Munich, Germany
[3] Med Univ Innsbruck, Dept Neurol, Innsbruck, Austria
[4] Helmholtz Zentrum Munchen, Inst Humangenet, Munich, Germany
[5] Fdn Aurora Onlus, Neuromuscular Omnictr Sud NEMO SUD, Messina, Italy
[6] Fdn Serena Onlus, Neuromuscular Omnictr NEMO, Milan, Italy
[7] Univ Milan, Dept Biochem Sci Hlth, Milan, Italy
[8] Schon Klin Munchen Schwabing, Munich, Germany
[9] Vivantes Klinikum Spandau, Berlin, Germany
[10] Tech Univ Munich, Inst Humangenet, Munich, Germany
[11] Catholic Univ, Inst Clin Biochem, Rome, Italy
[12] Niguarda Ca Granda Metropolitan Hosp, Ctr Study Rare Hereditary Dis, Milan, Italy
[13] Munich Cluster Syst Neurol, SyNergy, Munich, Germany
[14] Tech Univ Munich, Inst Human Genet, Klinikum Rechts Isar, Munich, Germany
来源
MOVEMENT DISORDERS | 2017年 / 32卷 / 04期
关键词
dystonia; exome; diagnostics; ANO3; ADCY5; DOPA-RESPONSIVE DYSTONIA; PRIMARY TORSION DYSTONIA; MOVEMENT-DISORDERS; MUTATIONS; GENE; DISEASE; CLASSIFICATION; PHENOMENOLOGY; GUIDELINES; DYSKINESIA;
D O I
10.1002/mds.26808
中图分类号
R74 [神经病学与精神病学];
学科分类号
摘要
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. (C) 2016 International Parkinson and Movement Disorder Society.
引用
收藏
页码:549 / 559
页数:11
相关论文
共 50 条
  • [21] Melanoma follow-up and mortality: A large-scale study of Medicare patients
    Hashmi, Osama
    Waller, Jennifer
    Turrentine, Jake
    JOURNAL OF THE AMERICAN ACADEMY OF DERMATOLOGY, 2018, 79 (03) : AB190 - AB190
  • [22] TEN YEAR CLINICAL FOLLOW-UP OF YOUTH WITH EARLY ONSET PSYCHOSIS
    Gisela, Sugranyes
    De la Serna, Elena
    Redondo, Marina
    Ilzarbe, Daniel
    Castro-Fornieles, Josefina
    Baeza, Inmaculada
    SCHIZOPHRENIA BULLETIN, 2018, 44 : S125 - S125
  • [23] Whole-exome sequencing and immune profiling of early-stage lung adenocarcinoma with fully annotated clinical follow-up
    Kadara, H.
    Choi, M.
    Zhang, J.
    Parra, E. R.
    Rodriguez-Canales, J.
    Gaffney, S. G.
    Zhao, Z.
    Behrens, C.
    Fujimoto, J.
    Chow, C.
    Yoo, Y.
    Kalhor, N.
    Moran, C.
    Rimm, D.
    Swisher, S.
    Gibbons, D. L.
    Heymach, J.
    Kaftan, E.
    Townsend, J. P.
    Lynch, T. J.
    Schlessinger, J.
    Lee, J.
    Lifton, R. P.
    Wistuba, I. I.
    Herbst, R. S.
    ANNALS OF ONCOLOGY, 2017, 28 (01) : 75 - 82
  • [24] Risk factors for early-onset colorectal cancer: A large-scale Chinese cohort study
    Pan, Zhe
    Huang, Junfeng
    Huang, Mingkai
    Yao, Zhiyuan
    Huang, Jiongqiang
    Chen, Jingsong
    Yu, Xiaoli
    Wang, Rongchang
    JOURNAL OF THE NATIONAL CANCER CENTER, 2023, 3 (01): : 28 - 34
  • [25] Exome sequencing of multiplex bipolar disorder families and follow-up resequencing implicate rare variants in neuronal genes contributing to disease etiology
    Maaser, A.
    Strohmaier, J.
    Ludwig, K. U.
    Henschel, L.
    Streit, F.
    Degenhardt, F.
    Sivalingam, S.
    Schenk, L. M.
    Koller, A. C.
    Fischer, S. B.
    Thiele, H.
    Nuernberg, P.
    Guzman Parra, J.
    Orozco Diaz, G.
    Auburger, G.
    Albus, M.
    Borrmann-Hassenbach, M.
    Jose Gonzalez, M.
    Gil Flores, S.
    Cabaleiro Fabeiro, F. J.
    del Rio Noriega, F.
    Perez Perez, F.
    Haro Gonzalez, J.
    Rivas, F.
    Mayoral, F.
    Herms, S.
    Hoffmann, P.
    Cichon, S.
    Rietschel, M.
    Noethen, M. M.
    Forstner, A. J.
    EUROPEAN JOURNAL OF HUMAN GENETICS, 2019, 27 : 261 - 262
  • [26] FOLLOW-UP OF 27 CANDIDATE GENES FROM A WHOLE-EXOME SEQUENCING STUDY IN LARGE FAMILIES WITH BIPOLAR DISORDER BY RESEQUENCING OF AN INDEPENDENT PATIENT-CONTROL COHORT
    Fischer, Sascha
    Hoffmann, Per
    Reinbold, Celine
    Burger, Bettina
    Herms, Stefan
    Streit, Fabian
    Rivas, Fabio
    Mayoral, Fermin
    Parra, Jose Guzman
    Arias, Barbara
    Schulze, Thomas
    Rietschel, Marcella
    Noethen, Markus
    Forstner, Andreas
    Cichon, Sven
    EUROPEAN NEUROPSYCHOPHARMACOLOGY, 2021, 51 : E62 - E63
  • [27] Genetic landscape of recessive diseases in the Vietnamese population from large-scale clinical exome sequencing
    Ngoc Hieu Tran
    Thanh-Huong Nguyen Thi
    Hung-Sang Tang
    Le-Phuc Hoang
    Trung-Hieu Le Nguyen
    Nhat-Thang Tran
    Thu-Huong Nhat Trinh
    Van Thong Nguyen
    Bao-Han Huu Nguyen
    Hieu Trong Nguyen
    Loc Phuoc Doan
    Ngoc-Minh Phan
    Kim-Huong Thi Nguyen
    Hong-Dang Luu Nguyen
    Minh-Tam Thi Quach
    Thanh-Phuong Thi Nguyen
    Vu Uyen Tran
    Dinh-Vinh Tran
    Quynh-Tho Thi Nguyen
    Thanh-Thuy Thi Do
    Nien Vinh Lam
    Phuong Cao Thi Ngoc
    Dinh Kiet Truong
    Hoai-Nghia Nguyen
    Minh-Duy Phan
    Hoa Giang
    HUMAN MUTATION, 2021, 42 (10) : 1229 - 1238
  • [28] Cognitive impairment and level of functioning in early-onset psychosis: 8 years follow-up study
    Remberk, B.
    Bazynska, A. K.
    Rybakowski, F.
    Niwinski, P.
    EUROPEAN NEUROPSYCHOPHARMACOLOGY, 2012, 22 : S417 - S417
  • [29] Magnetic controlled growing rods for early-onset scoliosis: a 4-year follow-up
    Teoh, Kar Hao
    Winson, Daniel M. G.
    James, Stuart H.
    Jones, Alwyn
    Howes, John
    Davies, Paul R.
    Ahuja, Sashin
    SPINE JOURNAL, 2016, 16 (04): : S34 - S39
  • [30] Cognitive impairment in early-onset MS: A reappraisal after a 10-year follow-up
    Amato, MP
    Ponziani, G
    Pracucci, G
    Siracusa, G
    Sorbi, S
    NEUROLOGY, 1999, 52 (06) : A499 - A499
12345