LCR-MH: Study of BDNF Pathway Biomarkers in the Cerebrospinal Fluid in Patients With Huntington's Disease

Sponsor

University Hospital, Montpellier (Other)

Overall Status

Recruiting

CT.gov ID

NCT04012411

Collaborator

(none)

135

Enrollment

Location

Arms

51.9

Anticipated Duration (Months)

2.6

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

Huntington disease (HD, 1.3/10 000) is an autosomal dominant disease due to an abnormal expansion of CAG triplets in HTT gene.

Several pathophysiological mechanisms have been evoked, including an alteration of the signaling pathway of the Brain Derived Neurotrophic Factor (BDNF), a neurotrophic factor involved in the survival of neurons (striatal and hippocampal) and synaptic plasticity. BDNF is synthesized at the level of cortical neurons and transported, through the axonal transport in which the Htt is involved, to the nerve endings; it's then secreted in response to excitatory synaptic activity, especially at the level of glutamatergic synapses. Besides, at the postsynaptic level it binds with great specificity to TrkB receptors (tropomyosin-related kinase receptors B) with a neuroprotective effect on dendritic and axonal growth and an increase in synaptic plasticity, especially at the level of the striatum and the hippocampus.

BDNF is decreased in the brain of animal models, as well as in patients with HD; the alteration of this pathway would occur in the early stages of the disease.

In the context of concomitant multiple treatments, the BNDF pathway may be one of the therapeutic targets of HD.

Moreover, in HD it remains essential to detect biological markers representative of the different pathogenic pathways that can be tested in vivo in humans to confirm the hypotheses developed at the level of basic research; these biomarkers could subsequently become biomarkers of disease progression and/or biomarkers of therapeutic efficacy of potential targeted treatments.

Therefore, this study aims to characterize potential biomarkers of the BNDF pathway in plasma and CSF in subjects with HD and to confirm the importance of this pathogenic mechanism in vivo in humans.

Condition or Disease	Intervention/Treatment	Phase
Huntington Disease	Procedure: Brain MRI Procedure: Lumbar Punction Genetic: Blood sample Other: Cognitive evaluation	N/A

Detailed Description

Design: Multicentre prospective case-control study. Centres: University Hospital of Montpellier, France; University Hospital of Bordeaux, France; University Hospital of Nimes, France; University Hospital of Poitiers, France.
Main objective: To evaluate BDNF in cerebrospinal fluid as a potential marker of the BDNF-TrkB signaling pathway in vivo in HD patients at a symptomatic stage.
Secondary objectives: i) Evaluate plasma BDNF in subjects with HD; ii) Study the correlation between BDNF in CSF and BDNF in plasma; iii) Study the correlation between markers of the BDNF pathway and clinical severity, multimodal brain MRI parameters, and relevant markers of evolution of HD; iv) Confirm the increase of Tau and NFL (Neurofilament Light Chain) markers in plasma and in CSF, as markers of neuronal degeneration, in subjects with HD ; v) Test the TrkB assay in the CSF of patients with HD
Inclusion Criteria. General inclusion criteria: age ≥ 18 years old; national health insurance cover. Patient inclusion criteria: genetically confirmed Huntington's disease diagnosis (≥ 35 CAG repeat in HTT gene exon 1); written informed consent; patient agreement for LP, if requested. Control inclusion criteria: previous LP for medical reason; agreement for inclusion in a biobank for research purposes.
Exclusion Criteria. General exclusion criteria: subject protected by law, under curatorship or guardianship. Patients exclusion criteria: too severe HD, according to the clinician's judgment, possibly making difficult to perform cognitive evaluation or MRI; contraindications to brain MRI; contraindications to LP; inability to give informed consent. Control exclusion criteria: presence of a neurodegenerative of inflammatory central nervous system disease.
Inclusion period: 23 months
Duration of participation for each patient: 123 days maximum
Total research duration: 24 months
Plan of the study. Patients group: in 90 patients with HD, the investigators will perform: a collection of the main anamnestic and clinical data; a blood test for the determination of plasmatic BDNF, Tau and NFL and the genotyping of the Val66Met polymorphism of the BDNF gene; multimodal brain MRI with volumetry, diffusion tensor, functional MRI of rest; a measurement of the severity of Huntington's disease and Total Functional Capacity scales; neuropsychological tests (SDMT, STROOP test, Trail Making Test (TMT) A and B, digit span). In a subgroup of 45 patients, the investigators will also perform a lumbar puncture for the determination of BDNF, Tau, NFL and TrkB in CSF. Control Group: 45 controls will be selected from the samples present in the existing Biobank with CSF and plasma samples available in Montpellier, France. MRI data will be centralized and processed by the Imaging Institute I2FH Montpellier University Hospital.

Study Design

Study Type:

Interventional

Anticipated Enrollment :

135 participants

Allocation:

Non-Randomized

Intervention Model:

Parallel Assignment

Masking:

None (Open Label)

Primary Purpose:

Basic Science

Official Title:

Study of Brain Derived Neurotrophic Factor (BDNF) Pathway Biomarkers in the Cerebrospinal Fluid in Patients With Huntington's Disease

Actual Study Start Date :

Mar 3, 2020

Anticipated Primary Completion Date :

Jul 1, 2024

Anticipated Study Completion Date :

Jul 1, 2024

Arms and Interventions

Arm	Intervention/Treatment
Active Comparator: Patient with LP Huntington's disease patients who agreed to have LP	Procedure: Brain MRI Multimodal brain MRI: volumetry, diffusion tensor, functional rest MRI Procedure: Lumbar Punction Analysis of BDNF, Tau, NFL and TrkB in cerebrospinal fluid Genetic: Blood sample Analysis of BDNF, Tau, NFL, and Val66Met polymorphism Other: Cognitive evaluation Symbol Digit Modality Test (SDMT), Stroop test, Trail Making Test, Empan
Active Comparator: Patient without LP Huntington's disease patient with contraindication to LP or refusal to have LP	Procedure: Brain MRI Multimodal brain MRI: volumetry, diffusion tensor, functional rest MRI Genetic: Blood sample Analysis of BDNF, Tau, NFL, and Val66Met polymorphism Other: Cognitive evaluation Symbol Digit Modality Test (SDMT), Stroop test, Trail Making Test, Empan
No Intervention: Control Group Retrospective study with biologic samples of patients without Huntington's disease

Arm

Intervention/Treatment

Active Comparator: Patient with LP

Huntington's disease patients who agreed to have LP

Procedure: Brain MRI

Multimodal brain MRI: volumetry, diffusion tensor, functional rest MRI

Procedure: Lumbar Punction

Analysis of BDNF, Tau, NFL and TrkB in cerebrospinal fluid

Genetic: Blood sample

Analysis of BDNF, Tau, NFL, and Val66Met polymorphism

Other: Cognitive evaluation

Symbol Digit Modality Test (SDMT), Stroop test, Trail Making Test, Empan

Active Comparator: Patient without LP

Huntington's disease patient with contraindication to LP or refusal to have LP

Procedure: Brain MRI

Multimodal brain MRI: volumetry, diffusion tensor, functional rest MRI

Genetic: Blood sample

Analysis of BDNF, Tau, NFL, and Val66Met polymorphism

Other: Cognitive evaluation

Symbol Digit Modality Test (SDMT), Stroop test, Trail Making Test, Empan

No Intervention: Control Group

Retrospective study with biologic samples of patients without Huntington's disease

Outcome Measures

Primary Outcome Measures

BDNF(csf) in HD subjects compared to age-matched control subjects (+/- 5 years) [Inclusion]
centralized ELISA assay with Simoa - Quanterix kit technology at the Laboratory of Clinical Proteomic Biochemistry of Montpellier, France.

Secondary Outcome Measures

plasmatic BDNF in HD subjects vs controls [Inclusion]
Correlation between BDNF in CSF and BDNF in plasma [Inclusion]
Correlation between BDNF and disease parameters [Inclusion]
Correlation between BDNF in CSF or plasma and: disease severity, assessed through a Scale that quantifies the severity of the disease, the disease burden formula [(n.CAG-35.5) x age], the Total Functional Capacity functional scale (TFC), and cognitive scales (Symbol Digit Modalities Test, STROOP test, Trail Making test A and B, direct and indirect digit span); - MRI brain imaging: cerebral and striatal atrophy by morphological imaging, functional resting state MRI, and anatomical connectivity by diffusion tensor imaging
Total Tau and NFL levels in plasma and CSF in HD subjects vs control subjects [Inclusion]
TrkBcsf level in subjects with HD vs control subjects [Inclusion]

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years and Older

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Yes

Inclusion Criteria:

General inclusion criteria:
age ≥ 18 years-old
national health insurance cover
Patients inclusion criteria:
genetically confirmed Huntington's disease diagnosis (≥ 35 CAG repeat in HTT gene exon 1)
written informed consent
only for patients "with lumbar puncture (LP)": patient agreement for LP
Control inclusion criteria:
anterior LP for medical reason with consent for biobank "Neuro" with following samples present in this biobank : 2 mL blood + 0.5 mL plasma + 0.5 mL cerebrospinal fluid
information and non-opposition for the finality of this biobank
paired by age with a patient (+/- 5 years difference)

Exclusion Criteria:

General exclusion criteria:
protected by law
Patients exclusion criteria:
Huntington's disease stage too Evolved that may interfere with cognitive evaluations or MRI
contraindications to brain MRI
only for patients "with LP": contraindications to LP
incapacity to give informed consent
Control exclusion criteria:
neurodegenerative of inflammatory central nervous system pathology