Neuromelanin MRI: A Progression Marker in Early PD (InsIghtPD)

University of Nottingham

Status

Enrolling

Conditions

Progression, Disease

Parkinson Disease

Treatments

Diagnostic Test: MRI

Study type

Observational

Funder types

Other

Identifiers

NCT05631158

281685

Details and patient eligibility

About

Prospective observational study to qualify NM-MRI as progression marker in early Parkinson's.

Full description

Parkinson's is the second most common neurodegenerative disorder with progressive, disabling motor and non- motor symptoms for which effective symptomatic, but non disease-modifying treatment is available. Neuromelanin- containing neurons in the substantia nigra undergo neurodegeneration during Parkinson's disease. There is considerable heterogeneity in the progression of cell loss and clinical symptoms with major research interest in identifying prognostic subtypes.

A non-invasive biomarker that can track the loss of the neuromelanin-containing neurons would be highly desirable to (i) study subtype-specific trajectories of SN depigmentation, (ii) track disease progression in early Parkinson's to assist in stratifying groups and outcome assessment in clinical intervention trials, and (iii) enable patients and their families to better manage their condition including informed forward planning. Neuromelanin MRI (NM-MRI) is a new approach sensitive to the neuromelanin-iron complex, with proven association with the tissue changes of the number of the neuromelanin-containing neurons. Its diagnostic value was established in several studies case-control, but there is a lack of standardisation, multi-centre studies and prospective diagnostic trials. To date only a small, single arm retrospective study reported serial NM loss in Parkinson's.

Building on our previous work, the proposed research entails the development of an early progression biomarker for Parkinson's disease that is pathologically relevant, non-invasive, and uses MRI which is a widely available imaging method for detection. The experimental approach combines advanced computational imaging, retrospective use and extension of existing cohorts with a new dedicated prospective serial study using NM-MRI in uncertain parkinsonism, de novo and early Parkinson and healthy controls using latest MRI technology.

Enrollment

135 estimated patients

Sex

All

Ages

18 to 90 years old

Volunteers

Accepts Healthy Volunteers

Inclusion criteria

-Inclusion criteria for patients:

For Parkinson's patients and early-onset Parkinson's:
1. Diagnosis of Parkinson's disease, based on UK Brain Bank criteria and made within the preceding 3 years ('recent onset cases'); or
2. diagnosed at under 50 years ('under 50 years cases')
For clinical symptoms suspicious for a diagnosis of PD but clinical uncertainty with regard to a definite diagnosis:
1. clinical symptoms not meeting all of the required UK Brain Bank diagnostic criteria for the diagnosis of PD; or
2. clinical features not typically associated with PD and therefore raising the possibility of a different type disorder/movement disorder referred for a DaTSCAN as part of the National Health Service (NHS) clinical diagnostic work-up to investigate a suspicion for a parkinsonian movement disorder-type disease, or referred for a research DaTSCAN as part of existing N3iPD and PaMIR studies for the diagnostic work-up to investigate a suspicion for a parkinsonian movement disorder-type disease.
Age ≥18 to <90years
Being able and willing to provide informed consent

Inclusion criteria for healthy controls:

Age ≥18 to <90years
Being able and willing to provide informed consent

Exclusion criteria

Exclusion criteria for patients:
1. The patient has severe comorbid illness that would prevent full study participation
2. The patient has features indicating another type of degenerative parkinsonism, e.g. progressive supranuclear palsy
3. Drug-induced parkinsonism (Drug-unmasked PD is allowed)
4. Symmetrical lower body parkinsonism attributable to significant cortical and/or subcortical cerebrovascular disease (patients with 'incidental' small vessel disease on brain imaging are allowed).
5. Negative or normal functional imaging of the presynaptic dopamine system
6. The presence of UK Brain Bank exclusion criteria will be recorded at baseline, allowing for the presence of 1 or 2 exclusion criteria (e.g. dopamine antagonist Drug used; more than one affected relative) (if justified e.g. by abnormal SPECT).
7. Any contraindication to Magnetic Resonance (MR) scanning.
8. Any major neurological (other than PD), psychiatric or cardiovascular disease or history of brain injury.
9. Medical illness or medication that may affect brain morphometry or function.
10. Patient who is pregnant and/or breastfeeding.