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NCT01945567 Clinical Trial

Randomised Crossover Trial of DBS of Differential PSA Regions in Parkinson's Disease and Tremor

Parkinson's Disease Clinical Trial

Official title:
Randomised Crossover Trial of Deep Brain Stimulation of Differential Posterior Subthalamic Area Regions in Parkinson's Disease and Tremor

Clinical Trial Details — Status: Completed

Administrative data
NCT number NCT01945567
Other study ID # 2012-039
Secondary ID
Status Completed
Phase Phase 2
First received
Last updated
Start date August 2012
Est. completion date August 30, 2020

Study information
Verified date May 2021
Source The University of Western Australia
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The posterior subthalamic area holds promise as a target region for deep brain stimulation in tremor and Parkinson's disease. Using the magnetic resonance-directed implantable guide tube surgical technique, subregions of the posterior subthalamic area can be individually targetted on a single electrode lead trajectory. The hypothesis is that the caudal zona incerta may provide improved control of movement disorder symptoms than the more commonly stimulated dorsal zona incerta.

Description:

Randomisation between two treatment locations each programmed up to 3 milliamps in amplitude for 3 months: (1) caudal zona incerta and (2) dorsal zona incerta. This 6-month-long randomised phase is followed by 6 months of unblinded individualised empirically optimised settings programmed by a neurologist. Each of the three treatment periods ends with a full clinical, functional and quality of life assessment.

Recruitment information / eligibility
Status Completed
Enrollment 39
Est. completion date August 30, 2020
Est. primary completion date August 30, 2019
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: - Medication-refractory tremor and/or Parkinson's disease as defined by UK Brain Bank criteria with either inadequate control of motor fluctuations or dyskinesia despite optimised medical therapy Exclusion Criteria: - Significant cognitive, psychiatric and medical co-morbidities - Dementia with mini mental state examination score of less than 25/30 - Limited life expectancy due to a co-morbid condition

Study Design

Related Conditions & MeSH terms

Intervention

Device:
Up to 3 mA, 60 us, 130 Hz deep brain stimulation

Empirical unblinded deep brain stimulation programming

Locations
Country Name City State
Australia Sir Charles Gairdner Hospital Perth Western Australia

Sponsors (1)
Lead Sponsor Collaborator
The University of Western Australia

Country where clinical trial is conducted

Australia, 

Outcome
Type Measure Description Time frame Safety issue
Primary Change from baseline United Parkinsons Disease Rating Scale Part III at 3 months At end of first randomised crossover trial period 3 months
Primary Change from baseline United Parkinsons Disease Rating Scale Part III at 6 months At end of second randomised crossover trial period 6 months
Primary Change from baseline United Parkinsons Disease Rating Scale Part III at 12 months At end of non-randomised empirical deep brain stimulator programming period 12 months
Primary Change from baseline Fahn Tolosa Marin tremor scale at 3 months At end of first randomised crossover trial period for tremor patients 3 months
Primary Change from baseline Fahn Tolosa Marin tremor scale at 6 months At end of second randomised crossover trial period for tremor patients 6 months
Primary Change from baseline Fahn Tolosa Marin tremor scale at 12 months At end of empirical deep brain stimulator programming period for tremor patients 12 months
Secondary Change from baseline ON-OFF diary at 3 months For Parkinson's disease 3 months
Secondary Change from baseline ON-OFF diary at 6 months For Parkinson's disease 6 months
Secondary Change from baseline ON-OFF diary at 12 months For Parkinson's disease 12 months
Secondary Adverse events Any adverse medical event from date of randomization until the date of first documented adverse event or date of death from any cause, whichever came first, assessed up to 12 months 12 months
Secondary Change from baseline Short form 36 at 3 months At end of first randomised crossover period 3 months
Secondary Change from baseline Short form 36 at 6 months At end of second randomised crossover period 6 months
Secondary Change from baseline Short form 36 at 12 months At end of empirical deep brain stimulator programming period 12 months
Secondary Change from baseline Parkinsons Disease Quality of Life 39 at 3 months At end of first randomised crossover period for Parkinsons disease 3 months
Secondary Change from baseline Parkinsons Disease Quality of Life 39 at 6 months At end of second randomised crossover period for Parkinsons disease 6 months
Secondary Change from baseline Parkinsons Disease Quality of Life 39 at 12 months At end of empirical deep brain stimulator programming period for Parkinsons disease 12 months
Secondary Change from baseline L-dopa equivalent dose at 3 months At end of first randomised crossover period for Parkinsons disease 3 months
Secondary Change from baseline L-dopa equivalent dose at 6 months At end of second randomised crossover period for Parkinsons disease 3 months
Secondary Change from baseline L-dopa equivalent dose at 12 months At end of empirical deep brain stimulator programming period for Parkinsons disease 12 months
Secondary Change from baseline neuropsychological battery at 3 months At end of first randomised crossover period 3 months
Secondary Change from baseline neuropsychological battery at 6 months At end of second randomised crossover period 6 months
Secondary Change from baseline neuropsychological battery at 12 months At end of empirical deep brain stimulator programming period 12 months
Secondary Change from baseline verbal fluency at 3 months At end of first randomised crossover period 3 months
Secondary Change from baseline verbal fluency at 6 months At end of second randomised crossover period 6 months
Secondary Change from baseline verbal fluency at 12 months At end of empirical deep brain stimulator programming period 12 months
Secondary Change from baseline Mini-International Neuropsychiatric Interview Plus at 3 months At end of first randomised crossover period 3 months
Secondary Change from baseline Mini-International Neuropsychiatric Interview Plus at 6 months At end of second randomised crossover period 6 months
Secondary Change from baseline Mini-International Neuropsychiatric Interview Plus at 12 months At end of empirical deep brain stimulator programming period 12 months
Secondary Change from baseline United Parkinsons Disease Rating Scale parts I, II, IV, V at 3 months At end of first randomised crossover period for Parkinsons disease 3 months
Secondary Change from baseline United Parkinsons Disease Rating Scale parts I, II, IV, V at 6 months At end of second randomised crossover period for Parkinsons disease 6 months
Secondary Change from baseline United Parkinsons Disease Rating Scale parts I, II, IV, V at 12 months At end of empirical deep brain stimulator programming period for Parkinsons disease 12 months
Secondary Change from baseline Abnormal Involuntary Movement Scale at 3 months At end of first randomised crossover period for Parkinsons disease 3 months
Secondary Change from baseline Abnormal Involuntary Movement Scale at 6 months At end of second randomised crossover period for Parkinsons disease 6 months
Secondary Change from baseline Abnormal Involuntary Movement Scale at 12 months At end of empirical deep brain stimulator programming period for Parkinsons disease 12 months
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