## Abstract Parkinsonism in patients taking neuroleptic medications might be induced by dopamine receptor blockade alone or by dopamine blockade with nigrostriatal dysfunction. The differentiation between Parkinson's disease (PD) and drugโinduced parkinsonism (DIP) is difficult to assess on clinica
[123I] FP-CIT spect study in vascular parkinsonism and Parkinson's disease
โ Scribed by Jan Zijlmans; Andrew Evans; Flavia Fontes; Regina Katzenschlager; Svetoslav Gacinovic; Andrew J Lees; Durval Costa
- Publisher
- John Wiley and Sons
- Year
- 2007
- Tongue
- English
- Weight
- 212 KB
- Volume
- 22
- Category
- Article
- ISSN
- 0885-3185
No coin nor oath required. For personal study only.
โฆ Synopsis
Abstract
There is substantial evidence to support a role for small vessel disease (SVD) as a cause for vascular parkinsonism (VP). Using [^123^I] FPโCIT SPECT (single photon emission computed tomography), we have tried to determine whether VP patients have preโsynaptic dopaminergic function similar to PD patients, and whether the severity of parkinsonian symptoms as well as the levodopa response in VP patients are correlated with preโsynaptic dopaminergic dysfunction. Thirteen patients fulfilling operational clinical criteria for VP had [^123^I] FPโCIT scans. Mean [^123^I] FPโCIT uptake in the basal ganglia was significantly lower in VP patients than in healthy controls, and the asymmetry index was not significantly different between these groups. In contrast, compared with the PD group, only the mean asymmetry index was significantly lower in VP patients. None of the parameters measured was significantly different between VP patients who had an insidious onset of parkinsonism (VPi) and those who had an acute onset (VPa). There was a significant correlation between the bilateral basal ganglia FPโCIT uptake reduction in the VP patients and UPDRS motor scores, but not with the mean % reduction in motor UPDRS after levodopa. We suggest that in the majority of VP patients, preโsynaptic dopaminergic function is reduced. The presence of a rather symmetrical FPโCIT uptake in the basal ganglia may help to distinguish VP from PD and could therefore be used as a criterion for the clinical diagnosis of VP. ยฉ 2007 Movement Disorder Society
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