Parkinson's disease and iatrogenic impulsive-compulsive behaviors: A case/non-case study to build a complete model of individual vulnerability

Author:

Grall-Bronnec Marie12ORCID,Victorri-Vigneau Caroline23ORCID,Rouaud Tiphaine4ORCID,Verholleman Audrey1ORCID,Schreck Benoit12ORCID,Leboucher Juliette1ORCID,Thiabaud Elsa1ORCID,Feuillet Fanny25,Roy Monica4,Hardouin Jean-Benoit25ORCID,Guillou-Landreat Morgane67ORCID,Derkinderen Pascal48ORCID,Challet-Bouju Gaëlle12ORCID

Affiliation:

1. CHU Nantes, Addictology and Psychiatry Department, Nantes, France

2. Nantes Université, Univ Tours, CHU Nantes, CHU Tours, INSERM, MethodS in Patients centered outcomes and HEalth ResEarch, SPHERE, F-44000 Nantes, France

3. CHU Nantes, Pharmacology Department, Nantes, France

4. CHU Nantes, Neurology Department, Nantes, France

5. CHU Nantes, DRCI, Methodology and Biostatistic Department, Nantes, France

6. CHU Brest, Addictology Department, Nantes, France

7. Université de Bretagne Occidentale, ERCR SPURBO, Brest, France

8. Université de Nantes, Inserm U913, Nantes, France

Abstract

Abstract Background and aims Parkinson's disease (PD) is one of the most prevalent neurodegenerative diseases. First-line medications consist of drugs that act by counteracting dopamine deficiency in the basal ganglia. Unfortunately, iatrogenic impulsive-compulsive behaviors (ICBs) can occur in up to 20% of PD patients over the course of their illness. ICBs must be considered multifactorial disorders that reflect the interactions of the medication with an individual's vulnerability and the underlying neurobiology of PD. We aimed to explore the predictive genetic, psychopathological and neurological factors involved in the development of ICBs in PD patients by building a complete model of individual vulnerability. Methods The PARKADD study was a case/non-case study. A total of 225 patients were enrolled (“ICB” group, N =75; “no ICB” group, N =150), and 163 agreed to provide saliva samples for genetic analysis. Sociodemographic, neurological and psychiatric characteristics were assessed, and genotyping for the characterization of polymorphisms related to dopaminergic and opioid systems was performed. Results Factors associated with “ICBs” were younger age of PD onset, personal history of ICB prior to PD onset and higher scores on the urgency and sensation seeking facets of impulsivity. No gene variant was significantly associated, but the association with the opioid receptor mu 1 (OPRM1) rs1799971 polymorphism was close to significance. Discussion and conclusions The influence of gene-environment interactions probably exists, and additional studies are needed to decipher the possible role of the opioid system in the development of ICBs in PD patients.

Funder

French National Research Agency

Publisher

Akademiai Kiado Zrt.

Subject

Psychiatry and Mental health,Clinical Psychology,General Medicine,Medicine (miscellaneous)

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