BACKGROUND AND PURPOSE: Inherited prion diseases represent over 15% of human prion cases and are a frequent cause of early onset dementia. The purpose of this study was to define the distribution of changes in cerebral volumetric and microstructural parenchymal tissues in a specific inherited human prion disease mutation combining VBM with VBA of cerebral MTR and MD. MATERIALS AND METHODS: VBM and VBA of cerebral MTR and MD were performed in 16 healthy control participants and 9 patients with the 6-OPRI mutation. An analysis of covariance consisting of diagnostic grouping with age and total intracranial volume as covariates was performed. RESULTS: On VBM, there was a significant reduction in gray matter volume in patients compared with control participants in the basal ganglia, perisylvian cortex, lingual gyrus, and precuneus. Significant MTR reduction and MD increases were more anatomically extensive than volume differences on VBM in the same cortical areas, but MTR and MD changes were not seen in the basal ganglia. CONCLUSIONS: Gray matter and WM changes were seen in brain areas associated with motor and cognitive functions known to be impaired in patients with the 6-OPRI mutation. There were some differences in the anatomic distribution of MTR-VBA and MD-VBA changes compared with VBM, likely to reflect regional variations in the type and degree of the respective pathophysiologic substrates. Combined analysis of complementary multiparameter MR imaging data furthers our understanding of prion disease pathophysiology.
BACKGROUND AND PURPOSE: Inherited prion diseases represent over 15% of human prion cases and are a frequent cause of early onset dementia. The purpose of this study was to define the distribution of changes in cerebral volumetric and microstructural parenchymal tissues in a specific inherited human prion disease mutation combining VBM with VBA of cerebral MTR and MD. MATERIALS AND METHODS: VBM and VBA of cerebral MTR and MD were performed in 16 healthy control participants and 9 patients with the 6-OPRI mutation. An analysis of covariance consisting of diagnostic grouping with age and total intracranial volume as covariates was performed. RESULTS: On VBM, there was a significant reduction in gray matter volume in patients compared with control participants in the basal ganglia, perisylvian cortex, lingual gyrus, and precuneus. Significant MTR reduction and MD increases were more anatomically extensive than volume differences on VBM in the same cortical areas, but MTR and MD changes were not seen in the basal ganglia. CONCLUSIONS: Gray matter and WM changes were seen in brain areas associated with motor and cognitive functions known to be impaired in patients with the 6-OPRI mutation. There were some differences in the anatomic distribution of MTR-VBA and MD-VBA changes compared with VBM, likely to reflect regional variations in the type and degree of the respective pathophysiologic substrates. Combined analysis of complementary multiparameter MR imaging data furthers our understanding of prion disease pathophysiology.
Authors: Terrence R Oakes; Andrew S Fox; Tom Johnstone; Moo K Chung; Ned Kalin; Richard J Davidson Journal: Neuroimage Date: 2006-11-20 Impact factor: 6.556
Authors: Ramon Casanova; Ryali Srikanth; Aaron Baer; Paul J Laurienti; Jonathan H Burdette; Satoru Hayasaka; Lynn Flowers; Frank Wood; Joseph A Maldjian Journal: Neuroimage Date: 2006-10-27 Impact factor: 6.556
Authors: Gerard R Ridgway; Rohani Omar; Sébastien Ourselin; Derek L G Hill; Jason D Warren; Nick C Fox Journal: Neuroimage Date: 2008-09-20 Impact factor: 6.556
Authors: Mee-Ohk Kim; Leonel T Takada; Katherine Wong; Sven A Forner; Michael D Geschwind Journal: Cold Spring Harb Perspect Biol Date: 2018-05-01 Impact factor: 10.005
Authors: Kyan Younes; Julio C Rojas; Amy Wolf; Goh M Sheng-Yang; Matteo Paoletti; Gianina Toller; Eduardo Caverzasi; Maria Luisa Mandelli; Ignacio Illán-Gala; Joel H Kramer; Yann Cobigo; Bruce L Miller; Howard J Rosen; Michael D Geschwind Journal: Ann Clin Transl Neurol Date: 2021-05-05 Impact factor: 4.511
Authors: Enrico De Vita; Gerard R Ridgway; Mark J White; Marie-Claire Porter; Diana Caine; Peter Rudge; John Collinge; Tarek A Yousry; Hans Rolf Jager; Simon Mead; John S Thornton; Harpreet Hyare Journal: Neuroimage Clin Date: 2016-11-02 Impact factor: 4.881
Authors: Harpreet Hyare; Enrico De Vita; Marie-Claire Porter; Ivor Simpson; Gerard Ridgway; Jessica Lowe; Andrew Thompson; Chris Carswell; Sebastien Ourselin; Marc Modat; Liane Dos Santos Canas; Diana Caine; Zoe Fox; Peter Rudge; John Collinge; Simon Mead; John S Thornton Journal: Brain Commun Date: 2020-04-08