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Journal Article

Citation

Rehor G, Eiler M, Conca A. Psychiatr. Prax. 2008; 35(8): 404-405.

Vernacular Title

D3-Agonismus: Augmentierende Behandlungsmoglichkeit in der Tardiven Dyskinesie?

Affiliation

LKH Rankweil Abteilung für Psychiatrie I, Rankweil/Osterreich. gerald@rehor.at

Copyright

(Copyright © 2008, Georg Thieme Verlag)

DOI

10.1055/s-2008-1067380

PMID

18504692

Abstract

OBJECTIVE: Tardive dyskinesia (TD) is still a severe side effect induced by old neuroleptic drugs as well as modern atypical ones. The treatment is inefficient and often experimental. Aim of this study was to examine the effect of pramipexole, a dopamine D3 receptor agonist, in a severe case of oro-facial TD. METHOD: The TD of a 21 year old male patient with severe oro-facial occurrence was assessed by the Simpson et al scale before starting pramipexole therapy. Reevaluation was made during therapy and when the maximum dose of 1.44 mg a day was reached. Standard therapy with clozapine, valproic acid, oxazepam, bornaprin hydrochlorid and tiapride was continued as before. RESULTS: Oral dyskinesia decreased 20 % and no side effects were observed. Regarding psychopathology the patient was more interested in work and showed better concentration in therapies. CONCLUSION: Pramipexole could be a new promising add-on therapy in severe TD. Additionally, the low plasma binding and mild side effect profile of pramipexole makes it safe in combination with antipsychotic therapy.


Language: de

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