Putaminal diffusion tensor imaging measures predict disease severity across human prion diseases

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

doi:10.1093/braincomms/fcaa032

Putaminal diffusion tensor imaging measures predict disease severity across human prion diseases

Brain Commun. 2020 Apr 8;2(1):fcaa032. doi: 10.1093/braincomms/fcaa032. eCollection 2020.

Authors

Harpreet Hyare¹, Enrico De Vita², Marie-Claire Porter¹, Ivor Simpson³, Gerard Ridgway³, Jessica Lowe¹, Andrew Thompson¹, Chris Carswell¹, Sebastien Ourselin², Marc Modat², Liane Dos Santos Canas⁴, Diana Caine¹, Zoe Fox^{5

6}, Peter Rudge¹, John Collinge¹, Simon Mead¹, John S Thornton³

Affiliations

¹ MRC Prion Unit at UCL, Institute of Prion Diseases, London SE1 7EH, UK.
² Department of Biomedical Engineering, Centre for Medical Engineering, School of Biomedical Engineering & Imaging Sciences, King's College London, King's Health Partners, St Thomas' Hospital, London SE1 7EH, UK.
³ UCL Institute of Neurology, London, UK.
⁴ Centre for Medical Image Computing, UCL, London, UK.
⁵ Education Unit, UCL Institute of Neurology, London, UK.
⁶ UCL/UCLH Joint Research Office, London, UK.

Abstract

Therapeutic trials of disease-modifying agents in neurodegenerative disease typically require several hundred participants and long durations for clinical endpoints. Trials of this size are not feasible for prion diseases, rare dementia disorders associated with misfolding of prion protein. In this situation, biomarkers are particularly helpful. On diagnostic imaging, prion diseases demonstrate characteristic brain signal abnormalities on diffusion-weighted MRI. The aim of this study was to determine whether cerebral water diffusivity could be a quantitative imaging biomarker of disease severity. We hypothesized that the basal ganglia were most likely to demonstrate functionally relevant changes in diffusivity. Seventy-one subjects (37 patients and 34 controls) of whom 47 underwent serial scanning (23 patients and 24 controls) were recruited as part of the UK National Prion Monitoring Cohort. All patients underwent neurological assessment with the Medical Research Council Scale, a functionally orientated measure of prion disease severity, and diffusion tensor imaging. Voxel-based morphometry, voxel-based analysis of diffusion tensor imaging and regions of interest analyses were performed. A significant voxel-wise correlation of decreased Medical Research Council Scale score and decreased mean, radial and axial diffusivities in the putamen bilaterally was observed (P < 0.01). Significant decrease in putamen mean, radial and axial diffusivities over time was observed for patients compared with controls (P = 0.01), and there was a significant correlation between monthly decrease in putamen mean, radial and axial diffusivities and monthly decrease in Medical Research Council Scale (P < 0.001). Step-wise linear regression analysis, with dependent variable decline in Medical Research Council Scale, and covariates age and disease duration, showed the rate of decrease in putamen radial diffusivity to be the strongest predictor of rate of decrease in Medical Research Council Scale (P < 0.001). Sample size calculations estimated that, for an intervention study, 83 randomized patients would be required to provide 80% power to detect a 75% amelioration of decline in putamen radial diffusivity. Putamen radial diffusivity has potential as a secondary outcome measure biomarker in future therapeutic trials in human prion diseases.

Keywords: CJD; MRI; prion.

Abstract

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