Parkinson's Disease Clinical Trial
— CHEVALOfficial title:
Cholinesterase Inhibitors to Slow Progression of Visual Hallucinations in Parkinson's Disease:a Multi-center Placebo-controlled Trial.
Verified date | October 2018 |
Source | VU University Medical Center |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
Rationale: Visual hallucinations (VH) are the most common non-motor symptoms in Parkinson's
disease (PD). As an independent predictor for cognitive decline and nursing home placement
they form an important disability milestone in the course of PD. According to current
clinical guidelines minor VH do not require treatment per se. But as minor VH precede the
stage of major VH without insight and PD associated psychosis (PDP) they offer an opportunity
for early intervention. Neuroleptic drugs delay the transition into PDP but are unsuitable
for early treatment of VH due to their side effects. We hypothesize that cholinesterase
inhibitors (ChEI) are a well-tolerated alternative for the early treatment of minor VH to
delay the progression to PDP, and that brain network analysis is suitable to predict
treatment response.
Objective: Investigate whether early treatment with ChEI delays the progression of minor VH
to major VH without insight or PDP. In addition, we will measure motor control, psychotic
symptoms, cognitive impairment, mood disorders, daytime sleepiness, adverse events and
compliance, disability, caregiver burden and care use. We assess the cost-effectiveness of
early chronic treatment of VH with ChEI. Finally, we analyse changes of functional brain
networks before and during treatment.
Study design: A randomized, double blind, placebo-controlled, multi-center trial with an
economic evaluation.
Study population: 168 patients with PD and VH after fulfilling the in-and exclusion criteria.
Intervention: Rivastigmine capsule 6 mg BID or placebo BID for 24 months.
Main study parameters/endpoints: The primary outcome measure is the median time until PD
patients with minor VH progress to major VH without insight. The clinical endpoint is defined
as the start with antipsychotic treatment. Secondary outcome measures are changes in motor
control, psychotic symptoms, cognitive impairment, mood disorders, daytime sleepiness,
cholinergic deficiency, the number of adverse events, compliance, disability and caregiver
burden. The median time until PD patients with minor VH progress to PD dementia is measured
by means of changes in cognitive function. The secondary neurophysiological outcome measures
are peak frequency, functional connectivity, topological network organisation and the
direction of information flow. All relevant costs will be measured and valued.
Nature and extent of the burden and risks associated with participation, benefit and group
relatedness: The burden of participation consists of a total of 5 clinical visits (every 6
months), 5 telephone interviews on adverse events during the escalation phase and 9
questionnaires on health related costs (every 3 months). In a subgroup 3 additional visits
for EEG recording are needed. There is a risk for adverse reactions with rivastigmine
treatment; the most common are nausea and vomiting.
Status | Terminated |
Enrollment | 91 |
Est. completion date | September 2018 |
Est. primary completion date | September 2018 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 40 Years and older |
Eligibility |
Inclusion Criteria: - idiopathic PD with bradykinesia and at least two of the following signs; resting tremor, rigidity, and asymmetry (in accordance with clinical diagnostic criteria of the UK PD Society Brain Bank); - the presence of minor VH for at least 4 weeks, defined by a score of 1 or 2 on the hallucinations item of the Unified Parkinson's Disease rating Scale (UPDRS)1-MDS; - age 40 years and over. Exclusion Criteria: - Parkinson's Disease Psychosis, defined as the need for antipsychotic drug treatment in the opinion of the treating neurologist; - Parkinson's Disease Dementia, defined by a score < 24 on the Mini Mental State Examination (MMSE); - current delirium (caused by infection or metabolic disturbance); - current treatment with amantadine (Symmetrel) or anti-cholinergics, such as trihexyfenidyl (Artane) or biperideen (Akineton); - current or recent (<6 months) treatment with Cholinesterase inhibitor, such as rivastigmine (Exelon) or galantamine (Reminyl); - recent (<1 month) change in dopaminergic therapy; - history of psychosis or severe ophtalmologic disease (e.g. Charles Bonnet syndrome); - permanent stay in a nursing home; - no informed consent. |
Country | Name | City | State |
---|---|---|---|
Netherlands | Academic Medical Center | Amsterdam | |
Netherlands | University Medical Center Groningen | Groningen | |
Netherlands | Atrium Medical Center | Heerlen | |
Netherlands | University Medical Center St Radboud | Nijmegen |
Lead Sponsor | Collaborator |
---|---|
VU University Medical Center | Academisch Medisch Centrum - Universiteit van Amsterdam (AMC-UvA), Atrium Medical Center, International Parkinson Fonds Germany GmbH, Leiden University Medical Center, University Medical Center Groningen, University Medical Center Nijmegen, ZonMw: The Netherlands Organisation for Health Research and Development |
Netherlands,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | time to start with antipsychotic treatment for visual hallucinations | the time until Parkinson's disease patients with minor visual hallucinations progress to major visual hallucinations without insight (according to UPDRS 1 - MDS). The clinical endpoint is defined as the start with antipsychotic treatment. | 24 months | |
Secondary | motor control | change in motor control measured by UPDRS 3 - MDS | 24 months | |
Secondary | psychotic symptoms | change in occurence or severity of psychotic symptoms according to Scale of Assessment of Positive Symptoms (SAPS) and UPDRS 1 MDS. | 24 months | |
Secondary | cognitive function | change in cognitive function as measured by Mini Mental State Examination, Montreal Cognitive Assessment, Parkinson's Disease - Cognitive Rating Scale | 24 months | |
Secondary | mood disturbance | Mood disturbance according to the Hospital Anxiety and Depression Scale | 24 months | |
Secondary | daytime sleepiness | Daytime sleepiness on the Epworth Sleepiness Scale | 24 months | |
Secondary | cholinergic deficiency | Cholinergic deficiency, as a possible predictor for response to treatment, measured with the Cholinersterase Inhibitor Prognosticator | 24 months | |
Secondary | adverse events | Number and type of adverse events | 24 months | |
Secondary | compliance | Compliance to treatment measured by the number of remaining capsules after every 6 months of follow-up | 24 monhts | |
Secondary | disability | Disability based on the AMC Linear Disability Score | 24 months | |
Secondary | caregiver burden | Caregiver burden according to the Zarit Caregiver Burden Inventory | 24 months | |
Secondary | care use | Care use measured with the EuroQol-5D | 24 months | |
Secondary | EEG power analysis | peak frequency / relative power analysis | 12 months | |
Secondary | EEG functional connectivity | functional connectivity (phase lag index) | 12 months | |
Secondary | EEG topological network organisation | topological network organisation (minimum spanning tree) | 12 months | |
Secondary | EEG flow direction | direction of information flow (directed phase lag index) | 12 months | |
Secondary | EEG frequency band analysis | EEG analysis per frequency band | 12 months |
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