Abstract

The mechanisms of skeletal muscle atrophy, and the associated functional deficits, produced by a chronic decrease in the levels of neuromuscular activity are not well defined. Similarly, the most efficacious type or quantity of electro-mechanical activation to use as a countermeasure for these detrimental effects are undefined. We are proposing to use a model of virtually complete inactivity while preserving neurotrophic support, i.e., spinal cord isolation (SI), to address these issues. SI involves complete spinal cord transections at a mid-thoracic and high sacral level and bilateral dorsal rhizotomy between the two transection sites. SI, therefore, provides a baseline for determining the effects of chronic inactivity on skeletal muscle. We have successfully used a battery of molecular markers for protein metabolism to identify some of the major pathways involved in the skeletal muscle hypertrophic response associated with the functional overloading of a muscle by removal of its major synergists. These results have provided a framework for identifying the major pathways associated with muscle atrophy. Our overall working hypothesis is that the elimination of the normal activation/loading parameters on a muscle will down-regulate the pathways that have been shown to be up-regulated with increased activation/loading. We then will use high resistance isometric regimes to counteract the detrimental effects of inactivity on muscle function and phenotype. A unique BION stimulation implant system will be used to impose a known amount of electro-mechanical stimulation on the otherwise """"""""silent"""""""" plantarflexor muscles. Our approach will be to begin to identify the optimum stimulation paradigms for maximum maintenance of the properties of both a slow and a fast plantarflexor. We will vary the patterns of stimulation to optimize the normal contractile dynamics of each of these muscle types and will determine the effectiveness of imposing these electro-mechanical regimes once vs. twice per day. We will identify molecular mechanisms which can be used to counter the atrophic response. From a clinical perspective, understanding how critical molecular events can be modulated by known quantities of electro-mechanical stimulation will provide a clear direction for designing exercise and programmed mechanical stimulation paradigms to be used as preventive and/or rehabilitative tools for patients with muscle atrophy associated with spinal and neuromuscular maladies, aging, etc.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Program Projects (P01)
Project #
2P01NS016333-22
Application #
6777675
Study Section
Project Start
2003-07-16
Project End
2008-04-30
Budget Start
2003-07-16
Budget End
2004-04-30
Support Year
22
Fiscal Year
2003
Total Cost
$187,049
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Type
DUNS #
092530369
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Duru, Paul O; Tillakaratne, Niranjala J K; Kim, Jung A et al. (2015) Spinal neuronal activation during locomotor-like activity enabled by epidural stimulation and 5-hydroxytryptamine agonists in spinal rats. J Neurosci Res 93:1229-39
Tillakaratne, Niranjala J K; Duru, Paul; Fujino, Hidemi et al. (2014) Identification of interneurons activated at different inclines during treadmill locomotion in adult rats. J Neurosci Res 92:1714-22
Terson de Paleville, Daniela; McKay, William; Aslan, Sevda et al. (2013) Locomotor step training with body weight support improves respiratory motor function in individuals with chronic spinal cord injury. Respir Physiol Neurobiol 189:491-7
Johnson, Will L; Jindrich, Devin L; Roy, Roland R et al. (2012) Quantitative metrics of spinal cord injury recovery in the rat using motion capture, electromyography and ground reaction force measurement. J Neurosci Methods 206:65-72
Harkema, Susan; Behrman, Andrea; Barbeau, Hugues (2012) Evidence-based therapy for recovery of function after spinal cord injury. Handb Clin Neurol 109:259-74
Johnson, Will L; Jindrich, Devin L; Zhong, Hui et al. (2011) Application of a rat hindlimb model: a prediction of force spaces reachable through stimulation of nerve fascicles. IEEE Trans Biomed Eng 58:3328-38
Roy, Roland R; Zhong, Hui; Monti, Ryan J et al. (2011) Selectively reshaping a muscle phenotype: functional overload of cat plantaris. Muscle Nerve 43:489-99
Ichiyama, Ronaldo M; Broman, Jonas; Roy, Roland R et al. (2011) Locomotor training maintains normal inhibitory influence on both alpha- and gamma-motoneurons after neonatal spinal cord transection. J Neurosci 31:26-33
Joseph, M Selvan; Bilousova, Tina; Zdunowski, Sharon et al. (2011) Transgenic Mice With Enhanced Neuronal Major Histocompatibility Complex Class I Expression Recover Locomotor Function Better After Spinal Cord Injury. J Neurosci 89:365-372
Kim, Jung A; Roy, Roland R; Kim, Soo J et al. (2010) Electromechanical modulation of catabolic and anabolic pathways in chronically inactive, but neurally intact, muscles. Muscle Nerve 42:410-21

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