Dopaminergic denervation and associated MRI microstructural changes in the nigrostriatal projection in early Parkinson’s disease patients

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作者
M. López-Aguirre
M. Matarazzo
J. Blesa
M. H. G. Monje
R. Rodríguez-Rojas
A. Sánchez-Ferro
J. A. Obeso
J. A. Pineda-Pardo
机构
[1] HM CINAC (Centro Integral de Neurociencias Abarca Campal). Hospital Universitario HM Puerta del Sur,PhD Program in Physics
[2] HM Hospitales,Ken and Ruth Davee Department of Neurology
[3] Complutense University of Madrid,Department of Neurology
[4] Centro de Investigación Biomédica en Red de Enfermedades Neurodegenerativas (CIBERNED),Department of Medicine
[5] Instituto de Salud Carlos III,undefined
[6] Aligning Science Across Parkinson’s (ASAP) Collaborative Research Network,undefined
[7] Northwestern University,undefined
[8] Feinberg School of Medicine,undefined
[9] University Hospital 12 de Octubre,undefined
[10] Complutense University of Madrid,undefined
[11] University CEU-San Pablo,undefined
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Loss of dopaminergic neurons in the substantia nigra pars compacta (SNc) and a profound reduction of striatal dopamine are two hallmarks of Parkinson’s disease (PD). However, it’s unclear whether degeneration starts at the neuronal soma or the striatal presynaptic terminals, and how microstructural degeneration is linked to dopaminergic loss is also uncertain. In this study, thirty de novo PD patients and twenty healthy subjects (HS) underwent 6-[18F]-fluoro-L-dopa (FDOPA) PET and MRI studies no later than 12 months from clinical diagnosis. FDOPA uptake rate (Ki), fractional volume of free-water (FW), and iron-sensitive R2* relaxometry were quantified within nigrostriatal regions. Inter-group differences (PD vs HS) were studied using non-parametric statistics and complemented with Cohen’s d effect sizes and Bayesian statistics. Correlation analyses were performed exploring biomarker dependencies and their association with bradykinesia scores. PD patients exhibited a significant decline in nigrostriatal dopaminergic activity, being post-commissural putamen (−67%) and posterolateral SNc (−11.7%) the most affected subregions within striatum and SNc respectively. Microstructural alterations (FW) were restricted to the hemisphere corresponding to the most affected side and followed similar spatial gradients as FDOPA Ki (+20% in posterior putamen and +11% in posterolateral SNc). R2* revealed no relevant significant changes. FDOPA and FW were correlated within the posterolateral SNc, and clinical severity was associated with FDOPA Ki loss. The asymmetry between striatal and SNc changes for both dopaminergic depletion and microstructural degeneration biomarkers is consistent with a neurodegenerative process that begins in the striatal terminals before progressing toward the cell bodies in the SNc.
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