DATACOMT: Compensation Mechanisms in Parkinson's Disease

Sponsor

Assistance Publique - Hôpitaux de Paris (Other)

Overall Status

Completed

CT.gov ID

NCT02869945

Collaborator

(none)

Enrollment

Location

Arms

Actual Duration (Months)

0.9

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

Parkinson's disease onset is clinically defined as the appearance of motor symptoms including akinesia, tremor and hypertonia. Several studies have shown that motor symptoms occur when at least 50 % of dopaminergic neurons are lost. However, there are evidence suggesting that the level of dopaminergic denervation is not homogenous at the time of diagnosis.

Some patients have a higher level of dopaminergic loss at disease onset indicating the existence of compensation mechanisms. The aim of this study is to decipher how the metabolism of dopamine is involved in this compensation with a focus on the polymorphism of the COMT gene. This gene is expressed according to two variant: (i) COMT H that encodes a form of the enzyme with a high level of activity and (ii) COMT L that encode a form of the enzyme with a low level of activity. Thus, there are 3 possible genotypes in the population: (i) COMT HH associated with an increased degradation of dopamine, (ii) COMT LL associated with a decreased degradation of dopamine and (iii) COMT HH (intermediary between COMT HH and COMT LL).

The hypothesis is that this polymorphism of the COMT gene may participate to compensation mechanisms in early PD. Patients with COMT HH genotype may have an earlier motor symptoms onset than patients with COMT LL genotype.

To test this hypothesis, we will recruit 51 patients with de novo PD will be recruited (17 patients for each genotype). Given the distribution of COMT polymorphism in the population, a maximum sample of 76 patients will be screened to recruit 17 patients for each genotype.

Clinical evaluation will include MDS-UPDRS, Non Motor Symptoms Scale, segmental symptoms scale, Montreal Cognitive assessment, MMSE, Frontal assessment battery and Parkinson's disease behavioral assessment scale (ECMP). All the patients will have a monophotonic emission tomography with I-123-Ioflupane in order to assess the level of dopaminergic denervation and an MRI scan with resting state study. Cerebrospinal fluid sampling will be optional and will allow direct measurements of dopamine metabolites.

The main outcome measure will be the level of dopaminergic denervation on I-123-Ioflupane scans according to COMT genotype, age, gender and severity of motor symptoms on the MDS-UPDRS part 3.

If this hypothesis is confirmed, this will allow to test the efficacy of COMT inhibitors in order to delay dopaminergic drugs initiation for PD patients.

Condition or Disease	Intervention/Treatment	Phase
Parkinson Disease	Genetic: Identification of COMT HH, COMT HL or COMT LL genes Other: Brain MRI with resting state scan Other: Brain MPET	N/A

Detailed Description

The aim of this study is to decipher how the metabolism of dopamine is involved in this compensation with a focus on the polymorphism of the COMT gene. This gene is expressed according to two variants: (i) COMT H that encodes a form of the enzyme with a high level of aactivity and (ii) COMT L that encode a form of the enzyme with a low level of activity. Thus, there are 3 possible genotypes in the population: (i) COMT HH associated with an increased degradation of dopamine, (ii) COMT LL associated with a decreased degradation of dopamine and (iii) COMT HH (intermediary between COMT HH and COMT LL).

To test this hypothesis, 51 patients with de novo PD will be included (17 patients for each genotype). Given the distribution of COMT polymorphism in the population, a maximum sample of 76 patients will be screened for inclusion of 17 patients for each genotype.

Only untreated patients will be included in the study in order to have a reliable assessment of motor severity without interference of dopaminergic drugs.

The study will be scheduled as follow:

At the first visit (V1), inclusion criteria will be checked and patients will sign the informed consent. COMT genotype of selected patients will be analyzed.
Result of COMT genotype will be obtained within 4 weeks. Only the 17 first patients with each genotype will continue the study
For these patients, an evaluation visit with clinical assessment including MDS-UPDRS, Non Motor Symptoms Scale, segmental symptoms scale, Montreal Cognitive assessment, MMSE, Frontal assessment battery and Parkinson's disease behavioral assessment scale (ECMP) will be performed..

All the patients will have a monophotonic emission tomography with I-123-Ioflupane in order to assess the level of dopaminergic denervation. An MRI scan with resting state study will also be performed to assess the compensation mechanisms at the networks level. Cerebrospinal fluid sampling will be optional and will allow direct measurements of dopamine metabolites.

The main outcome measure will be the level of dopaminergic denervation on I-123-Ioflupane scans according to COMT genotype with and without adjustment for age, gender and severity of motor symptoms on the MDS-UPDRS part 3.

Secondary outcome measures will include:

level of dopaminergic denervation compared across the 3 genotypes (COMT HH, COMT HL and COMT HH) with and without adjustment for age, gender and motor scores
determination of functional compensation at the networks scale assessed on fMRI resting state scan according to dopaminergic denervation
determination of CSF dopamine metabolite profile at the time of diagnosis (CSF sampling will be optional).

If this hypothesis is confirmed, this will allow to test the efficacy of COMT inhibitors in order to delay dopaminergic drugs initiation for PD patients.

Study Design

Study Type:

Interventional

Actual Enrollment :

50 participants

Allocation:

Non-Randomized

Intervention Model:

Parallel Assignment

Masking:

Triple (Participant, Care Provider, Outcomes Assessor)

Primary Purpose:

Basic Science

Official Title:

Dopaminergic Denervation and COMT Polymorphism in de Novo Patients With Parkinson's Disease

Actual Study Start Date :

Sep 1, 2016

Actual Primary Completion Date :

Jul 1, 2021

Actual Study Completion Date :

Jul 1, 2021

Arms and Interventions

Arm	Intervention/Treatment
Other: COMT HH COMT HH gene	Genetic: Identification of COMT HH, COMT HL or COMT LL genes COMT HH, COMT HL or COMT LL genes identification Other: Brain MRI with resting state scan MRI scan with resting state study to be performed to assess the compensation mechanisms at the networks level. Other: Brain MPET Monophotonic emission tomography with I-123-Ioflupane to assess the level of dopaminergic denervation.
Other: COMT HL COMT HL gene	Genetic: Identification of COMT HH, COMT HL or COMT LL genes COMT HH, COMT HL or COMT LL genes identification Other: Brain MRI with resting state scan MRI scan with resting state study to be performed to assess the compensation mechanisms at the networks level. Other: Brain MPET Monophotonic emission tomography with I-123-Ioflupane to assess the level of dopaminergic denervation.
Other: COMT LL COMT LL gene	Genetic: Identification of COMT HH, COMT HL or COMT LL genes COMT HH, COMT HL or COMT LL genes identification Other: Brain MRI with resting state scan MRI scan with resting state study to be performed to assess the compensation mechanisms at the networks level. Other: Brain MPET Monophotonic emission tomography with I-123-Ioflupane to assess the level of dopaminergic denervation.

Arm

Intervention/Treatment

Other: COMT HH

COMT HH gene

Genetic: Identification of COMT HH, COMT HL or COMT LL genes

COMT HH, COMT HL or COMT LL genes identification

Other: Brain MRI with resting state scan

MRI scan with resting state study to be performed to assess the compensation mechanisms at the networks level.

Other: Brain MPET

Monophotonic emission tomography with I-123-Ioflupane to assess the level of dopaminergic denervation.

Other: COMT HL

COMT HL gene

Genetic: Identification of COMT HH, COMT HL or COMT LL genes

COMT HH, COMT HL or COMT LL genes identification

Other: Brain MRI with resting state scan

MRI scan with resting state study to be performed to assess the compensation mechanisms at the networks level.

Other: Brain MPET

Monophotonic emission tomography with I-123-Ioflupane to assess the level of dopaminergic denervation.

Other: COMT LL

COMT LL gene

Genetic: Identification of COMT HH, COMT HL or COMT LL genes

COMT HH, COMT HL or COMT LL genes identification

Other: Brain MRI with resting state scan

MRI scan with resting state study to be performed to assess the compensation mechanisms at the networks level.

Other: Brain MPET

Monophotonic emission tomography with I-123-Ioflupane to assess the level of dopaminergic denervation.

Outcome Measures

Primary Outcome Measures

Comparison of the degree of presynaptic dopaminergic denervation across the 3 genotypes group (COMT HH, COMT HL and COMT LL) at the time of diagnostic of Parkinson disease [Within 3 months after inclusion]
The degree of presynaptic dopaminergic denervation estimated by the potential links of 123I-FP-CIT (radioligand dopamine transporter) on scintigraphy images of single photon emission

Secondary Outcome Measures

Degree of presynaptic denervation in three groups: COMT HH, COMT LL, COMT HL with and without adjustment for age, sex and UPDRS III score [Within 3 months after inclusion]
CSF dopamine metabolite levels at the time of diagnosis (CSF sampling will be optional) in the groups COMT HH, COMT HL and COMT LL [Within 3 months after inclusion]
Functional connectivity resting MRI Index obtained by full integration and graph theory based on genotypes (COMT HH, COMT LL, COMT HL) and denervation degree (MPET). [Within 3 months after inclusion]
MDS UPDRS-III motor score according to the genotypes (COMT HH, COMT LL, COMT HL) and denervation degree observed by MPET [Within 3 months after inclusion]

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years and Older

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Inclusion Criteria:

Man or woman ≥ 18 years old,
Caucasian origin
Parkinson's disease considered to be probable as defined by the criteria of UK Parkinson's disease Brain Bank (Hugues and coll 2002)
Absence of anti-parkinsonian medication
Patient affilied to a social security system
Signed information consent form

Exclusion Criteria:

Parkinsonian syndrome secondary to neuroleptics
Atypical parkinsonian syndrome such a multisystem atrophy, progressive supranuclear paralysis, dementia with levy bodies.
MRI contraindication (claustrophobia, not compatible mechanical heart valve MRI, pacemaker, cochlear implant, other body ferromagnetic objects, pregnancy) - MPET contraindication (pregnancy, feeding, hypersensitivity to ioflupane [123]
Patient under guardianship or trusteeship
Any other significant pathology that could prevent patient participation and achievement of planned examinations (except for lumbar puncture)
Patient participating or having participated in other biomedical research involving a drug in the three months prior to inclusion
Specific exclusion criteria if lumbar puncture is accepted by the patient: Anticoagulation or antiplatelet treatment; history of hemostasis disorders; platelets <150,000 mm3; TP <80%; TCA (patient / control)> 1.2.
Hypersensitivity to local anesthetics with amide link or to any of the excipients