Parkinson Disease Clinical Trial
Official title:
A Double-blind, Cross-over Comparison of Closed Loop Versus Conventional Deep Brain Stimulation of the Subthalamic Nucleus in the Treatment of Parkinson's Disease
Currently, treatment of Parkinson's Disease with deep brain stimulation (DBS) uses continuous high frequency stimulation. The investigators have previously shown that by controlling the stimulation using feedback from the brain and only delivering stimulation when needed side-effects like speech disturbance can be reduced. Here the investigators contrast conventional DBS with adaptive DBS while patients are awake and sleeping.
Parkinson's disease (PD) is the major neurological movement disorder in terms of both
prevalence and morbidity, and in associated health care and social care costs. In the United
Kingdom about 120,000 people are affected and associated costs are estimated at £ 2 billion
per year. The current gold standard treatment for PD is levodopa therapy, however its use is
limited by the development of motor complications in up to 80% of patients over a 5-10 year
period. This has led to a resurgence in functional neurosurgery for PD over the last three
decades.
Deep brain stimulation (DBS) is now accepted treatment for patients with severe PD and is
supported by the Food and Drug Administration in the USA and National Institute of Clinical
Excellence in the UK with trials providing evidence that it improves quality of life over
best medical treatment. However, due to partial efficacy and side effects its potential is
relatively limited and it has so far generally been restricted to patients with severe
disease and uncontrollable motor complications with medical therapy.
Currently DBS provides continuous and fixed stimulation, but this constant stimulation
promotes side-effects like speech disturbance. Research by the investigators has shown that
by controlling the stimulation and only delivering it when needed side-effects can be
reduced. To show this the investigators developed a form of adaptive DBS in which they
controlled how much stimulation is delivered by directly recording the brain's activity from
the electrode used for brain stimulation. This provides a feedback signal.
However, although adaptive DBS works in an acute research setting, there are still several
questions to be answered before it can be translated in to a durable therapy option. The main
remaining questions are whether the amelioration of Parkinsonian symptoms is maintained over
periods longer than an hour or so, and whether it is triggered when arousals occur during
sleep. The latter is important to ensure that mobility is maintained when turning in bed and
during bathroom visits.
The Investigators would like to contrast conventional (continuous) DBS with adaptive DBS when
the same patients with Parkinsons are treated while both awake and asleep. Thus they can
follow treatment effects during the day and at night, in sleep. Patients will receive the two
types of stimulation in randomised order. Patients will not be told which form of stimulation
is being applied and the main measures used to evaluate the outcome of the study will be
video-taped performance on a number of motor tasks and the video-taping of mobility during
arousals and awakenings from sleep. Assessment of video-tapes is desirable as assessors can
then be blind to the treatment being applied. Thus assessments should not be biased.
Patients will undergo our standard 2-part DBS implantation. The experiments will be performed
whilst the patients are inpatients between the two operations and will therefore not require
any extra procedures, extra hospital stay or incur delay in starting therapeutic DBS.
The DBS electrode has four contacts, and the electrodes are bilaterally implanted. Patients
will be requested to withhold their usual medication overnight so that they are first
assessed off medication on each morning. Each morning we will start with some screening. On
the first of day this will involve finding the best contact for adaptive stimulation on the
DBS electrode on the two sides. DBS stimulation will be evaluated in order to find the best
contact, voltage and stimulation settings for each individual patient. This assessment is
similar to the standard clinical procedure experienced by patients when seen as outpatients
following surgery. The investigators will confirm that the settings remain appropriate during
the morning screening on the next day.
The investigators will use our custom-built externalized research system (ERS) to allow
recordings and stimulation. The ERS will be affixed to the subject with sticky tape or a
bandage. The device is small and lightweight and communicates with a personal computer. The
electrical connections to the DBS leads will be through temporary extensions with appropriate
mechanical slack. The temporary extensions will be later replaced at stimulator implant with
new sterile extensions. To allow for stimulation return, a conductive clip to the ERS case
will be connected to a conducting (ECG) pad placed over chest. Periodic impedance checks will
ensure this connection is robust through the course of the experiment. The patient can be
ambulant whilst wearing the device. The safety of the ERS will be reviewed independently
prior to the start of the study.
Patients will be randomised as to whether they receive conventional DBS or adaptive DBS and
will then cross-over to the second type of stimulation. All procedures will be repeated in
matched form in the two treatment periods. The patient's usual medication will be started
once each screening test is completed and the medication continued through-out the day.
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