Cerebrovascular Accident Clinical Trial
Official title:
Dopamine Release in Use-Dependent Plasticity in Health and Disease
This study will examine how dopamine, a brain chemical, affects motor training. Taken by
mouth, dopamine can enhance motor training, especially during rehabilitation after brain
damage. The study will also examine whether Sinemet, a drug containing a precursor of
dopamine, can improve motor training.
Healthy normal volunteers and stroke patients between 18 and 80 years of age may be eligible
for this study. Healthy volunteers must be right-handed. Stroke patients must have had a
stroke that caused weakness in one hand, from which they have recovered enough to be able to
move the thumb in different directions. Participants will have up to three study sessions, as
follows:
Prestudy 1 (MRI, TMS with motor training)
- Session 1: Magnetic resonance imaging (MRI) of the brain. This procedure uses a strong
magnetic field and radio waves to show structural and chemical changes in tissues.
During the scan, the patient lies on a table in a narrow cylinder containing a magnetic
field. He or she can communicate with the staff administering the test at all times.
- Session 2: Transcranial magnetic stimulation (TMS) - The subject sits in a comfortable
chair with the right forearm held still at the side and the head held still by an
aluminum frame. A magnetic coil is placed over the head, and a small probe is attached
to the thumb to measure thumb movement. Magnetic pulses are occasionally delivered over
the scalp, likely inducing a mild thumb movement. After this test, the subject takes a
tablet of either Sinemet or placebo (a look-alike pill with no active ingredient). Fifty
minutes after taking the pill, the subject undergoes motor training that involves
performing brisk thumb movements at a rate of 1 movement per second. At the end of the
training, TMS is repeated.
- Session 3: Identical to session 2, except subjects who took Sinemet in session 2 now
take placebo, and vice versa.
Prestudy 2 (MRI, PET without motor training, no TMS)
- Session 1: MRI of the brain if the subject has not had one within the last 12 months.
- Session 2: Positron emission tomography (PET) scanning - This procedure provides
information on brain chemistry and function. First, the subject is given either Sinemet
or placebo. The subject lies on a bed in a doughnut-shaped machine with a custom-molded
plastic mask placed over the face and head to support the head and hold it still during
the scanning. A catheter (plastic tube) is placed in each arm-one to inject
[11C]raclopride-a radioactive substance that competes with dopamine for binding in
certain parts of the brain and can be detected by the PET scanner-and one to draw blood
samples for measuring the level of Sinemet in the blood.
- Session 3: Identical to session 2, except subjects who took Sinemet in session 2 now
take placebo, and vice versa.
Main Study (MRI, TMS, PET with motor training)
- Session 1: MRI of the brain, if one has not been done within the last 12 months.
- Session 2: TMS, followed by administration of Sinemet or placebo and PET scanning with
motor training. The subject lies quietly during the first half of the PET session and
performs brisk thumb movements during the second half. After completing the PET scan,
the subject undergoes TMS again.
- Session 3: Identical to session 2, except subjects who took Sinemet in session 2 now
take placebo, and vice versa.
It has been proposed that the nigrostriatal and cortical dopaminergic systems are involved in
motor learning in health and disease. However, it is not known to which extent dopamine
influences use-dependent plasticity (UDP), one of the crucial functions that mediate recovery
of motor function after stroke. Understanding the role of dopamine on UDP in healthy
volunteers and patients with stroke may impact the development of rationale strategies to
promote functional recovery after this condition.
The aim of the present protocol is to provide evidence for the influence of dopaminergic
function on UDP in health and disease. We plan to address this issue in two different,
complementary ways (main experiment): (a) determine if UDP is positively correlated with the
decrease in raclopride binding potential (RAC-BP) in the contralateral dorsal striatum
(primary outcome measure), and (b) determine if administration of a dopaminergic drug will
enhance UDP and elicit a decrease in RAC-BP in the contralateral dorsal striatum.
Before the main experiment, we will assess the ability of a dopaminergic drug to enhance UDP
(prestudy 1, motor training only), and the effects of a dopaminergic drug on RAC-BP during
resting condition (prestudy 2, RAC-PET during resting condition only).
UDP will be assessed using a technique developed in our lab, in which we have extensive
experience. In short, we will evaluate TMS-evoked thumb movement directions after a period of
motor training consisting of performance of voluntary thumb movements for 30 minutes.
Striatal and cortical dopamine release will be assessed with positron emission tomography
using the dopamine-D2 receptor radioligand [(11)C]raclopride, after administration of
placebo, and after administration of a dopaminergic drug. The study will be initially done in
a group of healthy volunteers and then in a group of patients with chronic subcortical stroke
who experienced good motor recovery.
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