Huntington's disease progression: PET and clinical observations

doi:10.1093/brain/122.12.2353

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Brain, Vol. 122, No. 12, 2353-2363, December 1999
© 1999 Oxford University Press

Review article

Huntington's disease progression

PET and clinical observations

Thomasin C. Andrews¹, Robert A. Weeks¹, Nora Turjanski¹, Roger N. Gunn¹, Laura H. A. Watkins³, Barbara Sahakian³, John R. Hodges⁴, Anne E. Rosser³, Nicholas W. Wood² and David J. Brooks¹^,2

¹ MRC Cyclotron Unit, Hammersmith Hospital, ² Institute of Neurology, London and ³ MRC Centre for Brain Repair, Addenbrooke's Hospital and ⁴ MRC Cognition and Brain Sciences Unit, Cambridge UK

Correspondence to: Dr Thomasin Andrews, MRC Cyclotron Unit, Imperial College School of Medicine, Hammersmith Hospital, Du Cane Road, London W12 0NN, UK E-mail: thom{at}cu.rpms.ac.uk

Using serial [¹¹C]SCH 23390- and [¹¹C]raclopride-PET, we havemeasured the rate of loss of striatal dopamine D1 and D2 receptorbinding over a mean of 40 months in nine asymptomatic adultHuntington's disease mutation carriers, four patients with symptomaticdisease, seven mutation-negative controls and three subjectsat risk for the disease. Eight of the nine asymptomatic Huntington'sdisease mutation carriers had serial [¹¹C]raclopride-PET andshowed a mean annual loss of striatal D2 binding of 4.0%. Onlyfive of these eight, however, showed active progression, andthey had a mean annual loss of D2 binding of 6.5%. All nineasymptomatic mutation carriers had serial [¹¹C]SCH 23390-PETand showed a mean annual loss of striatal D1 binding of 2.0%.Four of these subjects demonstrated active progression and theyhad a mean annual loss of 4.5%. Our four symptomatic Huntington'sdisease patients showed a mean annual loss of D2 binding of3.0% and of D1 binding of 5.0%. Loss of striatal D1 and D2 bindingwas significantly greater in the known mutation carriers thanin the combined at-risk and gene-negative groups (P < 0.05).At follow-up PET all subjects were clinically assessed usingthe Unified Huntington's Disease Rating Scale. Scores for motorfunction and total functional capacity correlated with PET measuresof striatal dopamine receptor binding both in the asymptomaticmutation carriers (D1, P < 0.01) and across the combinedasymptomatic and clinically affected Huntington's disease mutationcarrier group (D1 and D2, P < 0.001). We conclude that PETmeasures of striatal D1 and D2 dopamine binding can be usedto identify asymptomatic Huntington's disease mutation carrierswho are actively progressing and who would thus be suitablefor putative neuroprotective therapies. Measures of diseaseprogression rates in Huntington's disease patients and asymptomaticmutation carriers will be of critical importance in future trialsof experimental restorative treatments.

Huntington's disease; dopamine receptors; PET; disease progression; UHDRS

FDG = [¹⁸F]2-fluoro-2-deoxyglucose; TFC = total functional capacity; UHDRS = Unified Huntington's Disease Rating Scale

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