Imaging Studies of Cognitive Impairment in Parkinson s Disease
Status: | Completed |
---|---|
Conditions: | Cognitive Studies, Parkinsons Disease, Neurology |
Therapuetic Areas: | Neurology, Psychiatry / Psychology |
Healthy: | No |
Age Range: | 40 - Any |
Updated: | 3/14/2019 |
Start Date: | April 4, 2013 |
End Date: | February 3, 2015 |
Neural Correlates of Cognitive Impairment in Parkinson Disease
Background:
- Parkinson's disease causes slow movements, stiffness, and tremor. It can get worse over
time, and in some cases can lead to dementia. Researchers are interested in how dementia
affects the brain in people with Parkinson's disease. They will study both people with
Parkinson s disease and healthy volunteers. They will give tests of thinking and memory, and
look at brain activity using imaging studies. This may provide more information on what parts
of the brain are not working well in people who have dementia related to Parkinson's disease.
Objectives:
- To use imaging studies to see what parts of the brain do not work well in people with
dementia caused by Parkinson's disease.
Eligibility:
- Individuals at least 40 years of age who have Parkinson s disease.
- Healthy volunteers at least 40 years of age.
Design:
- Participants will be screened with a medical history and physical exam.
- This study requires two outpatient visits over 2 days.
- Participants will have tests of thinking, memory, and concentration. They will answer
questions and fill out questionnaires. The tests will also look at how quickly they can
move and handle small objects. The tests will take about 3 hours.
- Participants will have magnetic resonance imaging to study the brain. Functional MRI
(fMRI) can show what parts of the brain are used when performing a task. Participants
will respond to images on a computer screen during fMRI.
- Treatment will not be provided as part of this study.
- Parkinson's disease causes slow movements, stiffness, and tremor. It can get worse over
time, and in some cases can lead to dementia. Researchers are interested in how dementia
affects the brain in people with Parkinson's disease. They will study both people with
Parkinson s disease and healthy volunteers. They will give tests of thinking and memory, and
look at brain activity using imaging studies. This may provide more information on what parts
of the brain are not working well in people who have dementia related to Parkinson's disease.
Objectives:
- To use imaging studies to see what parts of the brain do not work well in people with
dementia caused by Parkinson's disease.
Eligibility:
- Individuals at least 40 years of age who have Parkinson s disease.
- Healthy volunteers at least 40 years of age.
Design:
- Participants will be screened with a medical history and physical exam.
- This study requires two outpatient visits over 2 days.
- Participants will have tests of thinking, memory, and concentration. They will answer
questions and fill out questionnaires. The tests will also look at how quickly they can
move and handle small objects. The tests will take about 3 hours.
- Participants will have magnetic resonance imaging to study the brain. Functional MRI
(fMRI) can show what parts of the brain are used when performing a task. Participants
will respond to images on a computer screen during fMRI.
- Treatment will not be provided as part of this study.
Objectives:
The purpose of this protocol is to identify the neural correlates of cognitive impairment in
Parkinson disease (PD) using magnetic resonance imaging (MRI).
Study Population:
We will study 36 PD patients, defined by the UK Parkinson s Society Brain Bank diagnostic
criteria [1], consisting of 12 patients with cognitively normal PD (PD-CogNL), 12 with PD
with mild cognitive impairment (PD-MCI) [2], and 12 with PD with dementia (PDD) [3]. We
will also study 12 age- and gender-matched healthy volunteers (HVs) as controls.
Design:
This is an observational study and includes 3 PD patient subgroups (PD-CogNL, PD-MCI and PDD)
and HVs group. Eligible participants will have one visit lasting 2- 4 days, ideally over 2
consecutive days. If the visit cannot be completed within that time frame, a second visit may
be scheduled within 3 months to complete the assessments. They will have a clinical
assessment, cognitive assessment, and MRI scans.
Outcome Measures and Hypothesis:
The primary outcome measure is the Mini-Mental State Examination (MMSE) score and
functional connectivity of cognitive networks, including default mode network, using
restingstate
functional MRI (fMRI). We hypothesize that there is a group difference in functional
connectivity of cognitive networks between the PD patient subgroups and HVs. We also
hypothesize that there is a correlation between the MMSE score and functional connectivity
of the default mode network in PD patients.
Secondary outcome measures are fractional anisotropy (FA) values, functional
connectivity of the cognitive networks during working memory tasks, olfactory function
score and the functional connectivity of olfactory network, and scales of brain perfusion and
the functional connectivity of default mode network. We hypothesize that there: 1) is a group
difference in FA values between PD patient subgroups and the HVs; 2) are group differences
in functional connectivity of the cognitive networks during the working memory task
between PD patient subgroups and HVs; 3) is a correlation between olfactory function and
functional connectivity of the olfactory network in patients with PD-CogNL or PD-MCI; and
4) are correlations between brain perfusion and the functional connectivity of the default
mode network in PD patients.
The purpose of this protocol is to identify the neural correlates of cognitive impairment in
Parkinson disease (PD) using magnetic resonance imaging (MRI).
Study Population:
We will study 36 PD patients, defined by the UK Parkinson s Society Brain Bank diagnostic
criteria [1], consisting of 12 patients with cognitively normal PD (PD-CogNL), 12 with PD
with mild cognitive impairment (PD-MCI) [2], and 12 with PD with dementia (PDD) [3]. We
will also study 12 age- and gender-matched healthy volunteers (HVs) as controls.
Design:
This is an observational study and includes 3 PD patient subgroups (PD-CogNL, PD-MCI and PDD)
and HVs group. Eligible participants will have one visit lasting 2- 4 days, ideally over 2
consecutive days. If the visit cannot be completed within that time frame, a second visit may
be scheduled within 3 months to complete the assessments. They will have a clinical
assessment, cognitive assessment, and MRI scans.
Outcome Measures and Hypothesis:
The primary outcome measure is the Mini-Mental State Examination (MMSE) score and
functional connectivity of cognitive networks, including default mode network, using
restingstate
functional MRI (fMRI). We hypothesize that there is a group difference in functional
connectivity of cognitive networks between the PD patient subgroups and HVs. We also
hypothesize that there is a correlation between the MMSE score and functional connectivity
of the default mode network in PD patients.
Secondary outcome measures are fractional anisotropy (FA) values, functional
connectivity of the cognitive networks during working memory tasks, olfactory function
score and the functional connectivity of olfactory network, and scales of brain perfusion and
the functional connectivity of default mode network. We hypothesize that there: 1) is a group
difference in FA values between PD patient subgroups and the HVs; 2) are group differences
in functional connectivity of the cognitive networks during the working memory task
between PD patient subgroups and HVs; 3) is a correlation between olfactory function and
functional connectivity of the olfactory network in patients with PD-CogNL or PD-MCI; and
4) are correlations between brain perfusion and the functional connectivity of the default
mode network in PD patients.
- INCLUSION CRITERIA:
For all subjects:
1. Age 40 or older.
2. Able to abstain from caffeine and alcohol for 24 hours before each visit.
3. English is the first language.
4. Right handed
For PD cohort:
1. Established diagnosis of PD.
2. History compatible with diagnosis of PD
3. Present with at least 3 of the following features: bradykinesia, resting tremor,
cogwheel rigidity or postural reflex impairment
4. One of the 3 clinical features is either bradykinesia or resting tremor
5. Currently taking or history of taking dopaminergic therapy with symptomatic response.
6. Is able to give informed consent or, if there is evidence of cognitive decline, able
to give assent and able to appoint a durable power of attorney (DPA) who can give
informed consent.
EXCLUSION CRITERIA for all subjects:
- Use of illegal drugs within the past 6 months.
- More than 7 alcoholic drinks a week for females or 14 alcoholic drinks a week for
males.
- History of a neurologic disorder such as a brain tumor, stroke, central nervous system
infection, multiple sclerosis, a movement disorder, epilepsy or a history of seizures,
except PD for PD patients.
- History of any head injury with loss of consciousness.
- Pregnancy or positive pregnancy test before the research procedure due to the risks
associated with MRI scans.
- Inability to lie flat on the back for up to 2 hours.
- Claustrophobia or a feeling of discomfort from being in small, enclosed spaces of
enough severity to prevent MRI scanning.
- Surgically or traumatically implanted metallic foreign bodies, such as pacemakers,
implanted medical pumps, implanted hearing aids, metal plates in the skull or metal
implants in the skull or eyes (other than dental fillings) that may be physically
hazardous during an MRI, or might distort the images.
- Ablative surgery or implanted electrodes and generator for deep brain stimulation
- Use of the following medications or substances within 6 months of getting MRI scan:
e.g., Cocaine, amphetamines, methylphenidate, ephedrine, phentermine, buproprion,
fentanyl, ketamine, and phencyclidine. Prescribed medication for common conditions,
such as allergy or cold, will not be exclusionary. Prescribed medication for PD will
not be exclusionary for PD patient.
- Have uncontrolled head movements that may impair image data collection (for PD
patients).
- Subjects with MMSE<26 for HVs.
- Have clinically relevant focal neurological findings on exam that suggest cerebral
pathology other than that associated with PD for PD patients.
- Any abnormal or focal finding on neurological exam for HVs.
- Abnormal findings in clinical MRI.
- PD patients with Beck Depression Inventory (BDI)-II > 31 will be excluded, because
severe or extreme depression may confound with cognitive function.
We found this trial at
1
site
9000 Rockville Pike
Bethesda, Maryland 20892
Bethesda, Maryland 20892
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