Facilitating Diagnostics and Prognostics of Parkinsonian Syndromes Using Neuroimaging

The University of Texas System (UT)

Status

Enrolling

Conditions

Multiple System Atrophy

Parkinson Disease

Progressive Supranuclear Palsy

Study type

Observational

Funder types

Other

Identifiers

NCT03872102

STU-2018-0428

Details and patient eligibility

About

The goals of this study are: 1) to identify biomarkers using neuroimaging that are associated with progression rate using statistical methods, and 2) to identify biomarkers that are associated with the differential diagnosis of Parkinson's disease and atypical parkinsonism.

Full description

Management of patients with parkinsonian symptoms has two critical gaps: (1) there are no clinically accepted biomarkers that may be used to inform disease progression rate in an individual with Parkinson disease (PD), and (2) no biomarkers exist to inform differential diagnosis of conditions that exhibit parkinsonian symptoms and signs. This 2-year study aims to develop a multi-modal neuroimaging biomarker that enables the prediction of disease progression rate in PD, and a biomarker that enables the differential diagnosis of PD, multiple systems atrophy (MSA), progressive supranuclear palsy (PSP), and healthy controls.

This study consists of two parts; neuroimaging of a defined population of mid to late stage PD subjects currently followed at UT Southwestern Medical Center, and recruitment of new subjects with PD, MSA, and PSP who will be followed clinically over 2 years and who will undergo neuroimaging.

Participants will be asked to undergo several types of neuroimaging which will be analyzed using machine learning techniques.

At each study visit of the newly recruited cohorts, appropriate clinical scales will be performed based on their diagnosis and used to track and measure disease severity and progression.

Enrollment

90 estimated patients

Sex

All

Volunteers

Accepts Healthy Volunteers

Inclusion criteria

For Aim 1:

Diagnosis of Parkinson disease
Existence of sufﬁcient clinical data from previous UTS Southwestern longitudinal study to determine progression rate (categorized as fast or slow)
Availability of suitable matched participant in the alternate progression group (fast or slow)
Willingness to participate in the imaging studies required for this study and to provide written informed consent

For Aim 2:

PD subjects will be recruited in accordance with the MDS Clinical Diagnostic Criteria for PD.

Duration of PD (since diagnosis) is < 5 years
Willing to participate in imaging and clinical scoring visits, and provide written informed consent
Subject and investigator agree that it is highly likely subject will be able to participate throughout the 2-year study period (no plans to move)

MSA subjects will be recruited in accordance with the Second Consensus Statement on Diagnosis of Multiple System Atrophy.

Duration of MSA (since diagnosis) is < 5 years
Willing to participate in imaging and clinical scoring visits, and provide written informed consent
Subject and investigator agree that it is highly likely subject will be able to participate throughout the 2-year study period (no plans to move away during the study)

PSP subjects will be recruited in accordance with the MDS Criteria for Diagnosis of Progressive Supranuclear Palsy and must meet the designation of "probable PSP" for inclusion.

Willing to participate in imaging and clinical scoring visits, and provide written informed consent
Subject and investigator agree that it is highly likely subject will be able to participate throughout the 2-year study period (no plans to move away during the study)

Control subjects will be recruited who meet the following criteria:

Roughly age and sex matched with the subjects in the PD cohort
No history or examination findings suggestive of any neurodegenerative disease
Normal gait, balance, and eye movements for age
No clinical evidence for symptomatic orthostatic hypotension
Willing to participate in imaging and clinical scoring visits, and provide written informed consent
Subject and investigator agree that it is highly likely subject will be able to participate throughout the 2-year study period (no plans to move away during the study)

Exclusion criteria

For Aims 1 and 2:

Any contraindications to undergoing the multimodal imaging program
All females of child-bearing potential, between the ages of 18-55, will be excluded from the study, unless they are confirmed to be not pregnant with a pregnancy test prior to scanning
This study will require constant clear communication throughout the duration of the study; therefore, non-English speakers will be excluded
Right-handed finger amputees
Cast on right hand or fingers at the time of enrollment
Has clinically significant liver, kidney, lung, metabolic or hormone disturbances which pose safety risk
Has a current clinically significant heart disease that poses a safety risk
Has a current clinically significant infectious disease or a medical comorbidity which poses a safety risk
Has a history of relevant severe drug allergy or hypersensitivity
Have a history of drug, alcohol, or substance dependence or abuse within the last year, or prior prolonged history of dependence or abuse
Currently undergoing chemotherapy or radiation for cancer
Recreational drug use in past six months
Central nervous systems disease or brain injury that would preclude participation in this study
Psychiatric or neurological disorder that would preclude participation in this study
Inability to keep or maintain research appointments

For Aim 1:

Severe disease progression such that participation in the imaging tests would be impossible or difficult
Non-availability of a suitable matched participant in the alternate progression group (fast or slow)

For Aim 2:

PD subjects

Unequivocal cerebellar abnormalities
Downward vertical gaze limitation or slowing of downward saccades
Diagnosis of behavioral variant frontotemporal dementia or primary progressive aphasia
Parkinsonian features restricted to the lower limbs for > 3 years
Treatment with dopamine blockers or depleters in a time course consistent with drug induced parkinsonism
Absence of an observable response to high dose levodopa despite moderate disease severity
Expert considers a diagnosis of alternative syndrome more likely than PD
Rapid progression of gait impairment requiring wheelchair within 5 years of onset
Complete absence of progression of motor symptoms over 5 years unless due to treatment
Early bulbar dysfunction within the first 5 years since diagnosis
Inspiratory respiratory dysfunction (stridor or frequent sighs)
Severe autonomic failure in the first 5 years
Recurrent falls (>1 per year) because of impaired balance in the first 3 years
Disproportionate dystonic anterocollis or hand contractures of hands or feet within 10 years
Absence of any of the common non-motor features of PD despite 5 years of disease
Otherwise unexplained pyramidal tract signs (weakness, hyperreflexia, or extensor toe signs)
Bilateral symmetric parkinsonism

MSA subjects

Clinically significant neuropathy
Hallucinations not induced by drugs
Onset after age 75 years
Family history of ataxia or parkinsonism
White matter lesions suggesting multiple sclerosis

PSP subjects

Predominant, otherwise unexplained impairment of episodic memory, suggestive of AD (Alzheimer's disease)
Predominant, otherwise unexplained autonomic failure, e.g., orthostatic hypotension (orthostatic reduction in blood pressure after 3 minutes standing > 30 mm Hg systolic or > 15 mm Hg diastolic), suggestive of multiple system atrophy or Lewy body disease
Predominant, otherwise unexplained visual hallucinations or fluctuations in alertness, suggestive of dementia with Lewy bodies
Predominant, otherwise unexplained multisegmental upper and lower motor neuron signs, suggestive of motor neuron disease (pure upper motor neuron signs are not an exclusion criterion)
Sudden onset or step-wise or rapid progression of symptoms, in conjunction with corresponding imaging or laboratory findings, suggestive of vascular etiology, autoimmune encephalitis, metabolic encephalopathies, or prion disease
History of encephalitis
Prominent appendicular ataxia
Identifiable cause of postural instability, e.g., primary sensory deficit, vestibular dysfunction, severe spasticity, or lower motor neuron syndrome

Control subjects

a. In the investigator's opinion, an unsuitable candidate to serve as a control

Trial design

90 participants in 2 patient groups

Aim 1: Develop a biomarker of PD disease progression rate

Description:

For Aim 1, we will enroll PD subjects spanning a range of progression rates that have been tracked at UT Southwestern Medical Center. Multimodal neuroimaging will be acquired from each subject. We will evaluate imaging data and known data on clinical progression using statistical techniques to determine a biomarker that associates with progression rate.

Aim 2: Develop a biomarker to distinguish between PD, PSP, MSA

Description:

For Aim 2, we will recruit subjects with PD, MSA, and PSP. We will also recruit healthy age/sex-matched controls. All subjects will complete a series of clinical assessments at three different time points, roughly 6-8 months apart: * Levodopa Equivalent Daily Dose * Parkinson disease questionnaire * Schwab and England ADL Scale * MDS-UPDRS (PD and healthy controls only) * UMSARS (MSA subjects only) * PSPRS (PSP subjects only) Multimodal neuroimaging will be acquired from each subject. We will evaluate imaging data from the participants along with prospectively collected information on clinical progression using statistical techniques to determine a biomarker that associates with the differentiation of PD, MSA, and PSP.

Trial contacts and locations

Central trial contact

Padraig E O'Suilleabhain, MD

Data sourced from clinicaltrials.gov

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