1. Sex differences in clinical and genetic determinants of levodopa peak-dose dyskinesias in Parkinson disease: an exploratory study
- Author
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Antonio Gambardella, Donatella Civitelli, Patrizia Tarantino, Mario Zappia, Elvira Valeria De Marco, Pierfrancesco Pugliese, Patrizia Spadafora, Aldo Quattrone, Sara Carrideo, Giuseppe Nicoletti, Ferdinanda Annesi, Grazia Annesi, Innocenza C. Cirò-Candiano, Gennarina Arabia, and Demetrio Messina
- Subjects
Male ,medicine.medical_specialty ,Levodopa ,Dyskinesia, Drug-Induced ,Genotype ,DNA Mutational Analysis ,behavioral disciplines and activities ,Central nervous system disease ,Antiparkinson Agents ,Cohort Studies ,Arts and Humanities (miscellaneous) ,Predictive Value of Tests ,Internal medicine ,mental disorders ,medicine ,Humans ,Genetic Predisposition to Disease ,Genetic Testing ,Age of Onset ,Psychiatry ,Genetic testing ,Aged ,Sex Characteristics ,DNA Repeat Expansion ,Polymorphism, Genetic ,medicine.diagnostic_test ,Dose-Response Relationship, Drug ,Receptors, Dopamine D2 ,Parkinson Disease ,Odds ratio ,medicine.disease ,nervous system diseases ,Dyskinesia ,Multivariate Analysis ,Female ,Neurology (clinical) ,Age of onset ,medicine.symptom ,Psychology ,Cohort study ,Sex characteristics ,medicine.drug - Abstract
Background Several factors, both clinical and genetic, may account for the risk of developing levodopa-induced peak-dose dyskinesias (PDD) in patients with Parkinson disease, but it is unclear how these factors interact for modulating the individual susceptibility for PDD. Objective To examine clinical and genetic risk factors for determining individual susceptibility of PDD in patients with Parkinson disease. Design Cohort study. Setting Referral center for Parkinson disease in Calabria, southern Italy. Patients Two hundred fifty patients with Parkinson disease were screened for the presence or absence of PDD following a short-term levodopa administration, and 215 subjects were available for further evaluations, including genotypic analysis of the CA dinucleotide short tandem repeat (CA n -STR) polymorphism located in the dopamine receptor D2 gene ( DRD2 ). Results One hundred five patients (48.8%) exhibited PDD following short-term levodopa administration, and 110 patients (51.2%) did not. Multivariate logistic regression analysis showed that independent predictors for the occurrence of PDD were female sex, earlier age at onset of Parkinson disease, longer duration of treatment, and higher dose of levodopa. Genetic factors related to the DRD2 CA n -STR polymorphism were not independent predictors for PDD in the total population, but they had a strong protective effect on the appearance of PDD when the multivariate analysis was performed in men (odds ratio, 0.34 [95% confidence interval, 0.14-0.84]). In women, a genetic protective effect on PDD was not evident. Conclusions Risk factors for PDD, both clinical and genetic, act in different ways for men and women. Genetic factors related to the DRD2 polymorphic status have a protective effect on PDD development in men but not in women. A female sex–related effect for the risk of PDD may be so strong that it overcomes any protective effect due to genetic factors.
- Published
- 2005
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