Abstract

Spinal motoneurons are essential for all movements. Their excitability is highly dependent on input from axons that originate in the brainstem and release the monoamines serotonin and norepinephrine. These neuromodulators facilitate strong persistent inward currents (PICs) in the dendrites of motoneurons, which enhance the effectiveness of synaptic input by as much as 6-fold. The loss of monoaminergic input to the distal spinal cord after spinal cord injury should thus tend to render motoneurons non-excitable. Yet, if motoneurons are non-excitable, why do spinal cord injury patients often suffer from debilitating spasms due to the presence of hyperexcitable, long-lasting spinal reflexes? This paradox has largely been resolved by recent studies of motoneurons following chronic injury of the sacral spinal cord of the rat. The motoneurons caudal to the injury site slowly re-develop the capacity to generate PICs over several weeks. Spasms develop in the affected musculature in the tail with the same post-injury time course as this recovery of the PICs. Thus, the redevelopment of PICs plays a primary role in the generation of spasticity in chronic injury. The goals of this proposal are to investigate the mechanisms of the post-injury re-development of motoneuron PICs (Aims 1 and 2) and to explore the implications of these mechanisms for drugs that could control spinal spasticity (Aims 3 and 4). All studies use the rat sacral cord chronic injury model, with the Aims 1 to 3 using an in vitro preparation that allows intracellular recordings and Aim 4 using awake animals with spastic tails.
Aim 1 considers the likelihood that motoneurons slowly become supersensitive to monoamines, so that the low levels of monoamines that persist post-injury begin to again facilitate the motoneuron PIC.
Aim 2 focuses on analyzing injury-induced changes in dendritic distribution and density of the ion channels generating the PICs. Such changes would contribute to PIC redevelopment and supersensitivity.
Aim 3 considers whether monoamine actions on motoneurons occur via different receptor subtypes than on interneurons. Finally, Aim 4 investigates the effectiveness of subtype specific monoaminergic agents on spasticity in the tails of chronically injury rats. These studies will not only enhance the understanding of cellular mechanisms of spasticity in spinal injury, but will also provide a basis for development of new pharmacological agents for therapeutic control of spasticity in human patients. ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
1R01NS047567-01A1
Application #
6823014
Study Section
Sensorimotor Integration Study Section (SMI)
Program Officer
Kleitman, Naomi
Project Start
2004-09-15
Project End
2009-04-30
Budget Start
2004-09-15
Budget End
2005-04-30
Support Year
1
Fiscal Year
2004
Total Cost
$244,877
Indirect Cost

  Institution

Name
University of Alberta
Department
Type
DUNS #
208095844
City
Edmonton
State
AB
Country
Canada
Zip Code
T6 2-E1

  Publications

Lucas-Osma, Ana M; Li, Yaqing; Lin, Shihao et al. (2018) Extrasynaptic ?5GABAA receptors on proprioceptive afferents produce a tonic depolarization that modulates sodium channel function in the rat spinal cord. J Neurophysiol :
Johnson, Michael D; Thompson, Christopher K; Tysseling, Vicki M et al. (2017) The potential for understanding the synaptic organization of human motor commands via the firing patterns of motoneurons. J Neurophysiol 118:520-531
Li, Yaqing; Lucas-Osma, Ana M; Black, Sophie et al. (2017) Pericytes impair capillary blood flow and motor function after chronic spinal cord injury. Nat Med 23:733-741
Thaweerattanasinp, Theeradej; Heckman, Charles J; Tysseling, Vicki M (2016) Firing characteristics of deep dorsal horn neurons after acute spinal transection during administration of agonists for 5-HT1B/1D and NMDA receptors. J Neurophysiol 116:1644-1653
Fenrich, Keith K; May, Zacincte; Torres-Espín, Abel et al. (2016) Single pellet grasping following cervical spinal cord injury in adult rat using an automated full-time training robot. Behav Brain Res 299:59-71
Li, Yaqing; Li, Lisa; Stephens, Marilee J et al. (2014) Synthesis, transport, and metabolism of serotonin formed from exogenously applied 5-HTP after spinal cord injury in rats. J Neurophysiol 111:145-63
D'Amico, Jessica M; Li, Yaqing; Bennett, David J et al. (2013) Reduction of spinal sensory transmission by facilitation of 5-HT1B/D receptors in noninjured and spinal cord-injured humans. J Neurophysiol 109:1485-93
D'Amico, Jessica M; Murray, Katherine C; Li, Yaqing et al. (2013) Constitutively active 5-HT2/ýý1 receptors facilitate muscle spasms after human spinal cord injury. J Neurophysiol 109:1473-84
Manuel, Marin; Li, Yaqing; Elbasiouny, Sherif M et al. (2012) NMDA induces persistent inward and outward currents that cause rhythmic bursting in adult rodent motoneurons. J Neurophysiol 108:2991-8
Murray, Katherine C; Stephens, Marilee J; Ballou, Edmund W et al. (2011) Motoneuron excitability and muscle spasms are regulated by 5-HT2B and 5-HT2C receptor activity. J Neurophysiol 105:731-48

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