Accelerated Diffusion MRI for Diagnosis of Hungtington Disease
NCT ID: NCT01884181
Last Updated: 2018-07-18
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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COMPLETED
80 participants
OBSERVATIONAL
2014-01-31
2017-12-31
Brief Summary
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1. Diffusion MRI using compressed sensing could have reduced motion sensitivity and improved susceptibility related artifact because of accelerated acquisition.
2. The macromolecule deposition in the brain of patients with Huntington Disease (HD) can lead to changes detectible by diffusion MRI.
To validate the hypothesis that the new accelerated diffusion MRI technique could produce a new biomarker for HD, patients with Huntington Disease will be recruited. The diffusion index will be calculated using accelerated acquisition. The diagnostic performance will be evaluated for data reconstructed with and without acceleration. The correlation with the disease severity will be assessed.
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Detailed Description
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Unfortunately the excessive motor abnormality such as chorea yields the acquisition of diffusion magnetic resonance imaging unfeasible in a clinical setting. The diffusion MRI with compressed sensing demonstrated reduced motion sensitivity and improved susceptibility related artifact because of the accelerated acquisition. Because of the reduced acquisition time, diffusion MRI in patient with Huntington Disease would be possible. It is therefore expected that the macromolecule deposition in the brain of patients with HD can lead to detectible changes in diffusion properties. The accelerated diffusion MRI techniques will be used to acquire data from healthy volunteers and patients with Huntington disease. The aim of the study is to develop and optimize a novel accelerated diffusion Magnetic Resonance Imaging (MRI) technique using advanced compressed sensing techniques. The joint sparsity constraint algorithm will be implemented in an in-line reconstruction platform for the diffusion MRI processing.
The second aim is to test the efficiency of the new accelerated diffusion MRI technique from phantom and in healthy human. Finally to validate the hypothesis that the new accelerated diffusion MRI technique could produce a new biomarker for HD, patients with Huntington Disease will be recruited. The diffusion index will be calculated using accelerated acquisition. The diagnostic performance will be evaluated for data reconstructed with and without acceleration. The correlation with the disease severity will be assessed. A risk management report will be concluded at the end of project execution for registration in the department of health. The acceleration diffusion MRI could provide new insight to the etiology of the disease. The in-line image reconstruction platform could be used for pediatric or psychiatric patients who cannot hold still in the scanner for a prolonged period and in patients with movement disorders.
Conditions
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Study Design
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CASE_CONTROL
PROSPECTIVE
Study Groups
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Huntington Disease Group
Established diagnosis by a neurological examination and genetic assessment of CAG expansion in the Htt gene.
No interventions assigned to this group
Healthy Controls
1. The healthy control subjects without a clinically significant neuropsychiatric disorders.
2. Able to understand and provide signed informed consent.
3. Age range and gender matched with Patients with Huntington Disease Group.
No interventions assigned to this group
Eligibility Criteria
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Inclusion Criteria
1. All participants should be aged between 20 and 70 year old.
2. Established diagnosis by a neurological examination and genetic assessment of CAG expansion in the Htt gene.
3. Able to understand and provide signed informed consent.
* Healthy Controls:
1. Able to understand and provide signed informed consent
2. age range and gender matched with Patients with HD
3. without significant neuropsychiatric disorders
Exclusion Criteria
1. Cardiac pacemaker implantation.
2. Implantation of intracranial metal device.
3. Significant major systemic disease, such as renal failure, heart failure, stroke, AMI/unstable angina, poor controlled diabetes mellitus, poor controlled hypertension.
4. Pregnant or breast feeding women.
5. Severe dementia.
6. Any documented abnormality of brain caused by etiologies other than HD by MRI and 18FDG PET studies, which might contribute to the cognitive function, such as hydrocephalus or encephalomalacia, will be excluded. Mild cortical atrophy will be allowed.
7. History of intracranial operation, including thalamotomy, pallidotomy, and/or deep brain stimulation.
8. Significant physical disorder or neuropsychiatric disorder.
20 Years
70 Years
ALL
Yes
Sponsors
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Wang . Jiun-Jie
OTHER
National Health Research Institutes, Taiwan
OTHER
Responsible Party
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Wang . Jiun-Jie
Professor
Principal Investigators
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Jiun-Jie Wang, PhD
Role: PRINCIPAL_INVESTIGATOR
ChangGung University
Locations
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ChangGung Memorial Hospital, Linkou
Taoyuan District, , Taiwan
Countries
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Other Identifiers
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102-1056B
Identifier Type: -
Identifier Source: org_study_id
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