Striatal (18F)dopa uptake in familial idiopathic dystonia

doi:10.1093/brain/116.5.1191

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Brain, Vol. 116, No. 5, 1191-1199, 1993
© 1993 Guarantors of Brain

research-article

Striatal (¹⁸F)dopa uptake in familial idiopathic dystonia

E. D. Playford¹, N. A. Fletcher², G. V. Sawle¹, C. D. Marsden² and D. J. Brooks¹^,2

¹MRC Cyclotron Unit, Clinical Sciences Section, Hammersmith Hospital London, UK ²Department of Clinical Neurology, Institute of Neurology, National Hospitals for Neurology and Neurosurgery London, UK

Correspondence to: Correspondence to Dr E. D Playford, MRC Cyclotron Unit, Hammersmith Hospital, DuCane Road, London W12OHS, UK

It is known that most cases of idiopathic torsion dystonia (ITD)are inherited in an autosomal dominant fashion. Despite clarificationof the underlying genetic defect, no consistent structural lesionhas been identified in ITD, and it is probable that a biochemicaldisturbance is the basis of the disorder.

To determine whether there is impaired function of the nigro-striataldopaminergic terminals in ITD we studied 11 subjects with generalizedITD and a positive family history using (¹⁸F)dopa and PET scanning.Of these 11 patients, eight had putamen (¹⁸F)dopa uptake withinthe lower half of the normal range, while three had uptake reducedby >2 SDs below the normal mean. The lowest putamen [¹⁸F]dopainflux constants were found in the most disabled patients. Asthese reductions were mild it is unlikely that abnormalitiesof the nigro-striatal dopaminergic pathway are the primary determinantof either the nature or the severity of dystonic symptoms.

In addition, we studied three presumed carriers of the ITD gene.These subjects all had normal striatal (¹⁸F)dopa influx constantssuggesting that (18F)dopa PET is unsuitable as a screening toolfor JTD.

Received October 5, 1992. Revised April 22, 1993. Accepted June 15, 1993.

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