BACKGROUND: TOR1A encodes a chaperone-like AAA-ATPase whose Delta GAG (Delta E) mutation is responsible for an early onset, generalised dystonia syndrome. Because of the established role of the TOR1A gene in heritable generalised dystonia (DYT1), a potential genetic contribution of TOR1A to the more prevalent and diverse presentations of late onset, focal dystonia has been suggested. RESULTS: A novel TOR1A missense mutation (c.613T-->A, p.F205I) in a patient with late onset, focal dystonia is reported. The mutation occurs in a highly evolutionarily conserved region encoding the AAA-ATPase domain. Expression assays revealed that expression of F205I or Delta E, but not wildtype TOR1A, produced frequent intracellular inclusions. CONCLUSIONS: A novel, rare TOR1A variant has been identified in an individual with late onset, focal dystonia and evidence provided that the mutation impairs TOR1A function. Together these findings raise the possibility that this novel TOR1A variant may contribute to the expression of dystonia. In light of these findings, a more comprehensive genetic effort is warranted to identify the role of this and other rare TOR1A variants in the expression of late onset, focal dystonia.
BACKGROUND:TOR1A encodes a chaperone-like AAA-ATPase whose Delta GAG (Delta E) mutation is responsible for an early onset, generalised dystonia syndrome. Because of the established role of the TOR1A gene in heritable generalised dystonia (DYT1), a potential genetic contribution of TOR1A to the more prevalent and diverse presentations of late onset, focal dystonia has been suggested. RESULTS: A novel TOR1A missense mutation (c.613T-->A, p.F205I) in a patient with late onset, focal dystonia is reported. The mutation occurs in a highly evolutionarily conserved region encoding the AAA-ATPase domain. Expression assays revealed that expression of F205I or Delta E, but not wildtype TOR1A, produced frequent intracellular inclusions. CONCLUSIONS: A novel, rare TOR1A variant has been identified in an individual with late onset, focal dystonia and evidence provided that the mutation impairs TOR1A function. Together these findings raise the possibility that this novel TOR1A variant may contribute to the expression of dystonia. In light of these findings, a more comprehensive genetic effort is warranted to identify the role of this and other rare TOR1A variants in the expression of late onset, focal dystonia.
Authors: N Brüggemann; N Kock; K Lohmann; I R König; A Rakovic; J Hagenah; A Schmidt; A Ziegler; H C Jabusch; H Siebner; E Altenmüller; A Münchau; C Klein Journal: Neurology Date: 2009-04-21 Impact factor: 9.910
Authors: J Hewett; C Gonzalez-Agosti; D Slater; P Ziefer; S Li; D Bergeron; D J Jacoby; L J Ozelius; V Ramesh; X O Breakefield Journal: Hum Mol Genet Date: 2000-05-22 Impact factor: 6.150
Authors: B Zirn; K Grundmann; P Huppke; J Puthenparampil; H Wolburg; O Riess; U Müller Journal: J Neurol Neurosurg Psychiatry Date: 2008-05-13 Impact factor: 10.154
Authors: D Sibbing; F Asmus; I R König; S Tezenas du Montcel; M Vidailhet; S Sangla; W H Oertel; A Brice; A Ziegler; T Gasser; O Bandmann Journal: Neurology Date: 2003-10-28 Impact factor: 9.910
Authors: Giovanni Defazio; Mar Matarin; Elizabeth L Peckham; Davide Martino; Enza M Valente; Andrew Singleton; Anthony Crawley; Maria Stella Aniello; Francesco Brancati; Giovanni Abbruzzese; Paolo Girlanda; Paolo Livrea; Mark Hallett; Alfredo Berardelli Journal: Mov Disord Date: 2009-03-15 Impact factor: 10.338
Authors: Fumiaki Yokoi; Janneth Oleas; Hong Xing; Yuning Liu; Kelly M Dexter; Carly Misztal; Melinda Gerard; Iakov Efimenko; Patrick Lynch; Matthew Villanueva; Raul Alsina; Shiv Krishnaswamy; David E Vaillancourt; Yuqing Li Journal: Neurobiol Dis Date: 2019-10-13 Impact factor: 5.996
Authors: Jasmin Hettich; Scott D Ryan; Osmar Norberto de Souza; Luís Fernando Saraiva Macedo Timmers; Shelun Tsai; Nadia A Atai; Cintia C da Hora; Xuan Zhang; Rashmi Kothary; Erik Snapp; Maria Ericsson; Kathrin Grundmann; Xandra O Breakefield; Flávia C Nery Journal: Hum Mutat Date: 2014-07-17 Impact factor: 4.878