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The Beneficial Effects of Naps on Motor Learning

The Beneficial Effects of Naps on Motor Learning

Recruiting
18-80 years
All
Phase N/A

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Overview

Background

Memory consolidation is the process by which memories become stable, long-term representations in the brain. Consolidation of a motor skill is dependent upon sleep. Some research shows that daytime naps improve people s motor performance and memory retention. Researchers want to find out how daytime naps may contribute to learning and support consolidation of motor skill memories.

Objective

To learn the role of memory replay during wakeful rest and sleep (naps) in retaining a newly learned skill.

Eligibility

English-speaking adults ages 18 and older with chronic stroke, or healthy, right-handed, English-speaking adults ages 18-35 and 50-80

Design

Participants will be screened with:

  • medical history
  • neurological history
  • medicine review
  • medical exam
  • neurological exam.

Participants will have a magnetic resonance imaging (MRI) scan of the brain. For this, they will lie down in a scanner. The scanner makes loud noises, so they will wear earplugs. They will fill out an MRI screening form before each MRI.

Participants will also have magnetoencephalography (MEG). MEG maps brain activity. It does this by recording the magnetic fields produced by naturally occurring electrical currents in the brain. For MEG, participants will lie down in the MEG room. Their eye movements may be recorded by a video camera.

Participants will have behavior testing. They will practice typing random keys. Then they will repeatedly type a custom sequence that they see on a computer screen. Then they will take a 2-hour nap. Then they will type the same sequence again.

Participants will have no more than 4 visits at the NIH over 3 months. Visits will last 2-4 hours each.

Description

Study Description:

We will investigate the within-individual contribution of wakeful and sleep neural replay to motor skill consolidation in three groups: (a) young healthy subjects, (b) older healthy subjects and (c) patients with chronic stroke.

Objective

The primary aim is to determine the relative contribution of neural replay during wakeful rest and sleep to consolidation of a newly learned skill in young and older healthy volunteers, and in chronic stroke patients with magnetoencephalography (MEG). The secondary aim is to evaluate differences in replay rates between these subject cohorts. We will also explore differences in replay rates, spatiotemporal dynamics of neural replay and sleep spindles to generate additional hypotheses and preliminary data for future studies.

Endpoints

The primary endpoint measure is motor skill consolidation (i.e., offline change in correct sequence typing speed following a nap). The secondary endpoint measure is neural replay rate. Exploratory endpoints measures are spatial (i.e. - parcellated source space) and time-frequency maps of neural replay during wakeful rest and sleep, and changes in button-press finger movement kinematics during learning.

Eligibility

  • HEALTHY VOLUNTEERS:

INCLUSION CRITERIA:

  • Age 18-35 (Arm 1) or 50-80 (Arm 2)
  • English speaking
  • Clear right-hand dominance (>74 on Edinburgh Handedness Inventory)
  • Normal neurological examination as determined by the screening clinician

EXCLUSION CRITERIA:

  • HCPS-section affiliated NIH staff
  • Current pregnancy
  • Contraindications for MRI or MEG.
  • Use of sleep medications within 24 hours of Experimental Session participation
  • Severe or progressive neurological, psychological or medical condition as determined by the screening clinician.

STROKE PATIENTS:

INCLUSION CRITERIA:

  • Age 18 or older
  • Willing and able to provide consent
  • Experienced a stroke 6 months ago or more that affected at least one of the upper extremities at time of stroke diagnosis
  • Ability to perform the study task as assessed during physical examination
  • English-speaking

EXCLUSION CRITERIA:

  • HCPS-affiliated NIH staff.
  • Current pregnancy
  • History of large stroke lesions in brainstem or cerebellum as determined by the screening clinician
  • Severe or progressive neurological disorder other than stroke (e.g., Parkinson s disease or multiple sclerosis) as determined by the screening clinician
  • Uncontrolled heart, lung, kidney, gastrointestinal, metabolic, psychiatric, sleep, or endocrine disorders as determined by the screening clinician
  • Contraindications for MRI or MEG.

Study details
    Stroke

NCT04312126

National Institute of Neurological Disorders and Stroke (NINDS)

24 June 2024

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