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Clinical Trial Details — Status: Not yet recruiting

Administrative data

NCT number NCT06213766
Other study ID # 69HCL23_1166
Secondary ID
Status Not yet recruiting
Phase N/A
First received
Last updated
Start date March 1, 2024
Est. completion date September 1, 2025

Study information

Verified date January 2024
Source Hospices Civils de Lyon
Contact Antoine GARNIER-CRUSSARD, Dr
Phone 04 72 43 20 50
Email antoine.garnier-crussard@chu-lyon.fr
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Spatial navigation is a high-level cognitive function that enables humans to orientate themselves and move around in space by constructing a mental representation of the environment. It is particularly interesting because it involves numerous neural networks, linked to proprioception and vision, for example. Despite the versatility of this cognitive function, spatial navigation is little studied clinically, although changes in spatial planning and navigation strategies have been associated with many brain disorders, including Alzheimer's disease (Coughlan et al., 2018). This may be explained in view of the neuropsychological tests currently in use, which do not effectively assess spatial navigation disorders. In addition, many non-pathological parameters - in particular socio-demographic and lifestyle - (Wolbers & Hegarty, 2010; Coutrot et al., 2018) affect spatial navigation performance. Separating the pathological component from these non-pathological factors in spatial navigation can be challenging. In this context, Sea Hero Quest (SHQ) has been developed (Coutrot et al., 2018; Spiers et al., 2021) as an international-scale cognitive spatial navigation task that holds great promise for assessing spatial navigation performance during normal and pathological ageing. SHQ is a video game that implements classic tasks from the spatial cognition literature, and has enabled the trajectories of 4 million players with varied socio-demographic profiles to be collected. In addition to the direct measurement of spatial displacements, eye movements, measured by eye-tracking, provide additional information on the cognitive processes associated with visual attention. The analysis of eye movements can provide valuable information about the strategies employed by humans during spatial navigation (Zhu et al., eLife 2023). While it is well known that normal ageing and pathological ageing (e.g. in the context of Alzheimer's disease) affect performance in simple spatial navigation or visual attention tasks, the neurocognitive mechanisms involved in this deterioration remain poorly understood. The investigators hypothesise that the joint analysis of ocular and spatial traces will provide a more detailed understanding of the cognitive strategies deployed during a spatial navigation task, and therefore of these underlying mechanisms. The investigators therefore propose to jointly study the association between two complementary cognitive functions: spatial navigation and visual attention, and their relationship with normal and pathological ageing (confirmed Alzheimer's disease, plasma biomarkers and genetic risk factors for Alzheimer's disease). The joint analysis of these different signals has never been carried out as part of research into normal ageing and Alzheimer's disease.


Recruitment information / eligibility

Status Not yet recruiting
Enrollment 250
Est. completion date September 1, 2025
Est. primary completion date September 1, 2025
Accepts healthy volunteers Accepts Healthy Volunteers
Gender All
Age group 20 Years to 85 Years
Eligibility Inclusion Criteria: Cognitively healthy subjects: - Participants aged between 20 and 85 years old; - Participant affiliated or entitled to a social security scheme; - Participants who have been informed and have given written consent. Patients with Alzheimer's disease: - Participant aged between 50 to 85 years old; - Participant undergoing memory clinic consultations for a diagnosed Alzheimer's disease, at the stage of minor neurocognitive impairment or major neurocognitive impairment, according to the NIA-AA 2011 criteria (McKahn et al., 2011, Albert et al., 2011); - Mild to moderate cognitive impairment, Mini-Mental State Examination (MMSE = 20/30, in the 6 months prior to inclusion); - Participant affiliated or entitled to a social security scheme; - Participants who have been informed and have given written consent. Exclusion Criteria: For all participants: - Severe, progressive or unstable pathology whose nature may interfere with the assessment variables (epilepsy, acute psychiatric or psychotic disorders, visual hallucinations, acute infection); - Consumption of toxic substances that may affect cognitive performance; - Deafness or blindness that could compromise the participant's assessment or participation in tasks and scales; - Participants under guardianship or legal protection; - Pregnant women, women in labour or breastfeeding mothers; - Persons under psychiatric care. Cognitively healthy subjects: - Participants diagnosed with a cognitive disorder. Specifically for patients with Alzheimer's disease: - Participants with a diagnosis other than Alzheimer's disease that promotes neurocognitive impairment (with the exception of cerebral microvascular involvement, i.e. mild to moderate microangiopathy); - Severe cerebral microangiopathy (extensive and severe white matter hypersignals, Fazekas score = 3); - Severe psycho-behavioral manifestations preventing performance of the task, at the investigator's discretion; - Current participation in an Alzheimer's disease drug research protocol, in particular testing 'disease-modifying' treatments that may interact with the pathophysiology of the disease (after randomisation).

Study Design


Related Conditions & MeSH terms


Intervention

Diagnostic Test:
Cognitive assessment
Group 1: Cognitively healthy subject: After signing the consent form, during the only visit of the study, the investigator will administer to cognitively healthy subjects two cognitive screening tests to ensure that they meet the criteria for group 1. If performance on the cognitive scales prove to be borderline or below current standards (Montreal Cognitive Assessment = 26/30 and MacNair Cognitive Difficulties Self-Rating Scale =15) for at least one of the 2 tests, the participant will prematurely end the study and may be offered an in-depth cognitive assessment as part of routine care. Group 2: Patients suffering from Alzheimer's disease: After signing the consent form, during the only visit of the study, the investigator will administer to patients the Montreal Cognitive Assessment to assess cognitive status.
Other:
Questionnaires
For every participants (group 1 and 2): During the only visit of the study and after the intervention 1, the participants will answer questionnaires about: Demographic data such as age, gender, weight, height, education level; Lifestyle habits such as usual mode of transport, sense of direction, use of GPS device, and video game practice; Quality of sleep over the previous month and the previous night; Cognitive reserve questionnaire from Rami et al., 2011; Concomitant treatment and comorbidities.
Device:
Spatial navigation task with eye-tracking.
For every participants (group 1 and 2): During the only visit of the study and after interventions 1 and 2, the participants will complete the spatial navigation task with eye-tracking. The participants will play the Sea Hero Quest video game and take on the role of the captain of a small boat that has to find its way through an aquatic environment. At the start of each level, the player is shown a map of the environment, with the boat's initial position and the buoys it must reach as quickly as possible in a set order. Once the map has been memorised, it disappears and the navigation begins. Participants will play 6 levels of Sea Hero Quest (two training levels and four different navigation levels). This intervention will be proposed by a trained team member and participants will play on a digital tablet connected to an eye-tracker. The total duration of the task is 30 min (training phase + assessment sequences).
Biological:
Blood sampling
For every participants (group 1 and 2): During the only visit of the study and after interventions 1, 2 and 3, a state-qualified nurse will take venous samples from 3 tubes of 4ml each. These blood samples will be frozen and stored until the end of the study when they will be analysed: Sample 1: plasmatic Quanterix p-tau217 assay; Sample 2: apolipoprotein E genotyping; Sample 3: measurement of plasmatic creatinine levels. Neither the cognitively healthy subjects, nor the patients, nor the clinicians in charge of the patients included will be informed of the results of these biological assays (absence of clinical interest established at the present time of the APOE genotype and the p-tau217 protein level, absence of modification of the care pathway, in adequacy to the bioethics law of August 02, 2021. Creatinine level is used in this study as an adjustment variable to interpret the p-tau217 protein level and will not be used for clinical interpretation.

Locations

Country Name City State
France Service de neuro-cognition et neuro-ophtalmologie Hôpital Pierre Wertheimer Bron
France Service de médecine du vieillissement - Hôpital Lyon Sud Pierre-Bénite
France Hôpital des Charpennes, Institut du Vieillissement, Hospices Civils de Lyon Villeurbanne Lyon

Sponsors (1)

Lead Sponsor Collaborator
Hospices Civils de Lyon

Country where clinical trial is conducted

France, 

Outcome

Type Measure Description Time frame Safety issue
Primary Analysis of spatial navigation strategies used by participants according to age. Spatial navigation strategies will be described thanks to machine learning identifying spatial navigation patterns taking into consideration:
Spatial performances: length of trajectories sampled at 2Hz (1 x-y coordinate every 500 ms) - the shorter the trajectory, the better the performance;
Eye movements: gaze sampling recorded and sampled at 60Hz to identify visual clues used by participants to solve the spatial task).
These patterns will be described according to participant's age.
Day 1 Just After inclusion
Secondary Cognitive health status: presence or absence of diagnosed Alzheimer's disease. Spatial navigation strategies will be compared according to participant's cognitive status (cognitively healthy versus Alzheimer's disease). Day 1 Just After inclusion
Secondary P-tau217 plasmatic protein assay in pg/mL interpreted in relation to creatinine levels and body mass index. Spatial navigation strategies will be compared according to the p-tau217 plasmatic protein assay. A Simoa (Single Molecule Array for Protein Detection) platform will use commercial kits to carry out the p-tau217 protein assay (Quanterix). Day 1 Just After inclusion
Secondary Genotyping of the apolipoprotein E gene: ApoE4 carrier or ApoE4 non carrier. Spatial navigation strategies will be compared according to the genotyping. A molecular biology platform will carry out genotyping for apolipoprotein E Day 1 Just After inclusion
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