Abstract

Increased age-related variability of motor function indicates that some older adults are more vulnerable to motor decline than others. Impaired motor function in vulnerable adults, leads to loss of ability to work and to lost independence, ultimately leading to substantially greater costs to an aging society. This proposal adopts a new and innovative approach to understanding motor function and motor fatigue (exercise induced reduction in strength) in vulnerable older men and women. We explore the large inter-subject variability that occurs with increased age to provide insight to a genetic mechanism underlying motor decline of the lower limb in men and women. Specifically, we associate inter-subject variability of motor function and fatigue with inheritance of the ?4 allele of the apolipoprotein-E (APOE) gene. We propose that APOE ?4 carriers have reduced effectiveness of the glutamate receptor (NMDA) in motor cortical areas and a subsequent reduction in intracortical excitability and lower neural drive during motor tasks than APOE ?4 non carriers: these mechanisms will be assessed with transcranial magnetic stimulation (TMS). Despite the substantive potential for intervention with vulnerable older adults, the cortical mechanisms underlying motor decline have received very limited attention. APOE ?4 inheritance is typically associated with risk of Alzheimer's Disease but was recently shown to increase the risk of motor function decline with advanced age. Whether motor fatigue during dynamic tasks, which is a common component of ergonomic and daily activities, exacerbates impaired strength and power in older adults with APOE ?4 inheritance is unknown. Thus, we hypothesize that impaired motor function and greater fatigue among older adults is related to possession of the APOE ?4 allele and mediated by reduced effectiveness of the glutamate receptor in motor cortical areas, reduced intracortical facilitation and decreased neural drive from motor cortical centers.
Aim 1 will determine whether APOE ?4 allele possession is associated with increased motor fatigue in lower limb muscles and decreased functionality of motor tasks (walking speed, balance, stair climbing) among independently living older men and women.
Aim 2 will compare intracortical facilitation and neural drive from the motor cortex during motor function tasks before and after motor fatigue among older men and women who are carriers and non-carriers of APOE ?4. Intracortical facilitation and supraspinal drive will be quantified with TMS of the motor cortex. Because older women are weaker and closer to functional performance thresholds without added vulnerability, sex differences will be explored to determine if older men or women are more vulnerable to motor impairment with APOE ?4 inheritance associated with reduced intracortical facilitation and supraspinal drive. The results will have high impact by: (1) providing insight into successful aging and the mediating role of intracortical facilitation and supraspinal drive; (2) identifying 'healthy' but vulnerable older adults for accelerated motor decline, and (3) providing a rationale for early, targeted strategies to offset altered neural networks and early motor decline.

Public Health Relevance

Healthy older men and women are a significant and rapidly growing part of the population and workforce, yet some are more vulnerable to motor decline than others. This proposal determines whether Apolipoprotein-E ?4 (APOE ?4) inheritance impairs lower limb muscle function and increases motor fatigue via reduced excitability within the brain and a subsequent loss of neural drive in independently living older men and women. We will also identify any apparent sex differences in muscle weakness, fatigue and reduced cortical excitability associated with APOE v4 inheritance among older adults. Identifying 'healthy' but sub-clinical older adults who are at risk for motor decline of lower limb muscles and a dominant neural mechanism, could significantly impact strategies to offset early motor decline in vulnerable older men and women and will provide insight into successful aging.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Exploratory/Developmental Grants (R21)
Project #
5R21AG045766-02
Application #
8891343
Study Section
Aging Systems and Geriatrics Study Section (ASG)
Program Officer
Wagster, Molly V
Project Start
2014-07-15
Project End
2016-05-31
Budget Start
2015-06-15
Budget End
2016-05-31
Support Year
2
Fiscal Year
2015
Total Cost
$186,016
Indirect Cost
$62,826

  Institution

Name
Marquette University
Department
Other Health Professions
Type
Schools of Allied Health Profes
DUNS #
046929621
City
Milwaukee
State
WI
Country
United States
Zip Code
53233

  Publications

Senefeld, Jonathon; Pereira, Hugo M; Elliott, Nicholas et al. (2018) Sex Differences in Mechanisms of Recovery after Isometric and Dynamic Fatiguing Tasks. Med Sci Sports Exerc 50:1070-1083
Senefeld, Jonathon; Yoon, Tejin; Hunter, Sandra K (2017) Age differences in dynamic fatigability and variability of arm and leg muscles: Associations with physical function. Exp Gerontol 87:74-83
Rozand, Vianney; Senefeld, Jonathon W; Hassanlouei, Hamidollah et al. (2017) Voluntary activation and variability during maximal dynamic contractions with aging. Eur J Appl Physiol 117:2493-2507
Hunter, Sandra K; Pereira, Hugo M; Keenan, Kevin G (2016) The aging neuromuscular system and motor performance. J Appl Physiol (1985) 121:982-995
Hunter, Sandra K; McNeil, Chris J; Butler, Jane E et al. (2016) Short-interval cortical inhibition and intracortical facilitation during submaximal voluntary contractions changes with fatigue. Exp Brain Res 234:2541-51
Hunter, Sandra K (2016) Sex differences in fatigability of dynamic contractions. Exp Physiol 101:250-5
Hunter, Sandra K (2016) The Relevance of Sex Differences in Performance Fatigability. Med Sci Sports Exerc 48:2247-2256