Clinical Trial: Evaluation of Nalmefene in Impulse Control Disorders in Parkinson's Disease: A Prospective Open Label Study

Study Status: Not yet recruiting
Recruit Status: Not yet recruiting
Study Type: Interventional

Official Title: Evaluation of Nalmefene in Impulse Control Disorders in Parkinson's Disease: A Prospective Open Label Study

Brief Summary:

Impulse control disorders (ICDs) (such as pathological gambling, hypersexuality, compulsive shopping …) are an increasingly recognized psychiatric complications in Parkinson's disease (PD). Therapeutic management of these disorders is important since they have an impact on patient quality of life. Dopamine agonists play a key role in the emergence of ICD.

Animal models and imaging underline the implication of opioid system in the genesis of ICD.

An opioid antagonist, the naltrexone, has been studied to treat ICDs in PD. Papay and al 2014 have found that patients treated by naltrexone showed an interesting decrease of their ICDs measured by the QUIP RScale. Nevertheless, naltrexone has shown adverse effects such as increasing hepatic liver enzymes. Nalmefene has no known hepatic adverse effects. Nalmefene is an opioid antagonist that has an antagonist action on μ and δ receptors, but also an agonist action on κ receptor. Grant and al 2006 has shown significant reduction of the severity of pathological gambling in patients treated with nalmefene.

The primary purpose is to evaluate the efficacy and the safety of nalmefene in the treatment of ICDs in PD.


Detailed Summary:

In this open study, 30 patients with ICDs, will be treated with 18 mg per day of nalmefene during 3 months.

Patients will be evaluated 2 times: at inclusion visit (J0) and 3 months after (at the end of the study, +3months).

At each time, patients will have :

  • a clinical and neurological evaluation
  • neuropsychological tests for cognitive, depression and TCI evaluations.
  • blood sample to test hepatic and renal functions
  • tolerance evaluation with a list of adverse events/effects

Patients will be contacted 3 times by phone: 2 weeks after inclusion, 1 month after inclusion and 2 months after inclusion, to note the presence of adverse events.


Sponsor: University Hospital, Clermont-Ferrand

Current Primary Outcome:

  • Tolerance of Nalmefene measured by the dropout rate secondary to adverse effects [ Time Frame: at + 3months ]
  • Efficacy of Nalmefene measured by the change from baseline of the QUIP-RS [ Time Frame: at + 3months ]


Original Primary Outcome: Same as current

Current Secondary Outcome:

  • Change from baseline of the cognitive state assessed by the Montreal Cognitive Assessment scale [ Time Frame: at +3 months ]
  • Change from baseline of the depression assessed by the Hamilton scale [ Time Frame: at +3 months ]
  • Change from baseline of the motor severity assessed by the Unified Parkinson Disease Rating Scale at +3 months [ Time Frame: at +3 months ]
  • Change from baseline of hepatic and renal function evaluated with blood samples at +3 months [ Time Frame: at +3 months ]


Original Secondary Outcome: Same as current

Information By: University Hospital, Clermont-Ferrand

Dates:
Date Received: October 14, 2016
Date Started: December 2016
Date Completion: May 2018
Last Updated: October 14, 2016
Last Verified: October 2016