Acute intermittent hypoxia enhances volitional elbow strength, and modulates spatial distribution of muscle activation patterns in persons with chronic incomplete spinal cord injury

Abstract

Background: Acute intermittent hypoxia (AIH) is an emerging technique for facilitating neural plasticity in individuals with major neurological deficits. In people with chronic incomplete spinal cord injury (iSCI), a single sequence of AIH enhances motor function such as hand grip strength and ankle plantarflexion torque, but the underlying mechanisms are not yet clear. Objective: To examine how AIH-induced changes in magnitude and spatial distribution of electromyography (EMG) activity over the surface of the biceps and triceps brachii muscles contributes to improved strength. Methods: Seven individuals with iSCI visited the laboratory on two occasions, at least a week apart, and received either AIH or Sham AIH intervention in a randomized order. AIH consisted of 15 brief (~60s) periods of low oxygen (fraction of inspired O2 = 0.09) alternating with 60s of normoxia, whereas Sham AIH consisted of repeated exposures to normoxic gas mixtures. Muscle activity of biceps and triceps brachii was recorded with high-density surface EMG during maximal elbow flexion and extension contractions. We used these EMG recordings to generate spatial maps which distinguished active muscle regions prior to and 60 minutes after AIH or Sham AIH. Results: After an AIH sequence, elbow flexion and extension forces increased by 91.7 +/- 33.5% and 51.7 +/- 21.9% from baseline, respectively, whereas there was no difference after Sham AIH exposure. Changes in strength were associated with an altered spatial distribution of EMG activity and increased root mean squared EMG amplitude in both biceps and triceps brachii muscles. Conclusions: These data suggest that altered motor unit activation profiles may underlie improved volitional strength after a single dose of AIH and warrant further investigation using single motor unit analysis techniques to further elucidate mechanisms of AIH-induced plasticity.

Competing Interest Statement

The authors have declared no competing interest.

Clinical Trial

NCT05513911

Funding Statement

This study was funded by the National Institute on Disability, Independent Living, and Rehabilitation Research

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Institutional Review Board office of Northwestern University gave ethical approval for this work

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Data Availability

All data produced in the present study are available upon reasonable request to the authors

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