Abstract

Neural processing in the vertebrate spinal cord is critically dependent on neuromodulatory input from the brainstem, which is dominated by the monoamines serotonin (5HT) and norepinephrine (NE). In motoneurons, monoamines act via G-protein coupled pathways to facilitate a very large persistent inward current (PIC) that is generated primarily in the dendrites. This PIC dominates the motoneuron's electrical behavior, amplifying synaptic input as much as 5 to 10 fold and allowing generation of long lasting behaviors like plateau potentials. In essence, the cell is switched from a state of passive dendritic integration to having its behavior dominated by highly active dendrites. Monoaminergic input to the cord is very diffuse, affecting many motor pools simultaneously. This highly excitable state has been considered to be very stable. Does such a generalized state of high excitability cause widespread co-contraction? We propose instead that the net effect of monoaminergic input is to dramatically increase the sensitivity of motoneurons to a very specific input, the reciprocal inhibition evoked by antagonist muscle length changes. Because reciprocal inhibition suppresses the PIC, the degree to which dendrites integrate actively or passively becomes highly sensitive to joint rotation. As a result, the descending monoaminergic systems should promote not co-contraction but reciprocal movement patterns. All studies are carried out using voltage clamp techniques in an in vivo preparation with a natural level of brainstem monoaminergic input.
In Aim 1, we consider what types of inhibition can control the PIC.
Aim 2 focuses on how excitatory and inhibitory synaptic inputs interact in the control of the PIC.
In Aims 3 and 4, we combine natural 3D movements of the hindlimb generated by a robotic arm with voltage clamp of motoneurons. This novel approach allows us to directly measure the coupling between muscle length and active dendritic integration via the PIC. The results will be directly relevant to spinal injury, in which monoaminergic input is severely disrupted. Drugs that mimic monoaminergic actions may restore the delicate balance required to control the interaction between movement and motoneuron electrical properties.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
2R01NS034382-09A1
Application #
6870091
Study Section
Sensorimotor Integration Study Section (SMI)
Program Officer
Chen, Daofen
Project Start
1999-09-30
Project End
2008-11-30
Budget Start
2004-12-01
Budget End
2005-11-30
Support Year
9
Fiscal Year
2005
Total Cost
$331,181
Indirect Cost

  Institution

Name
Northwestern University at Chicago
Department
Physiology
Type
Schools of Medicine
DUNS #
005436803
City
Chicago
State
IL
Country
United States
Zip Code
60611

  Publications

Wei, Kunlin; Glaser, Joshua I; Deng, Linna et al. (2014) Serotonin affects movement gain control in the spinal cord. J Neurosci 34:12690-700
Heckman, C J; Johnson, Michael D (2014) Reconfiguration of the electrical properties of motoneurons to match the diverse demands of motor behavior. Adv Exp Med Biol 826:33-40
Tysseling, Vicki M; Janes, Lindsay; Imhoff, Rebecca et al. (2013) Design and evaluation of a chronic EMG multichannel detection system for long-term recordings of hindlimb muscles in behaving mice. J Electromyogr Kinesiol 23:531-9
Johnson, Michael D; Kajtaz, Elma; Cain, Charlette M et al. (2013) Motoneuron intrinsic properties, but not their receptive fields, recover in chronic spinal injury. J Neurosci 33:18806-13
Frigon, Alain; Thibaudier, Yann; Johnson, Michael D et al. (2012) Cutaneous inputs from the back abolish locomotor-like activity and reduce spastic-like activity in the adult cat following complete spinal cord injury. Exp Neurol 235:588-98
Schuster, J E; Fu, R; Siddique, T et al. (2012) Effect of prolonged riluzole exposure on cultured motoneurons in a mouse model of ALS. J Neurophysiol 107:484-92
Gogliotti, Rocky G; Quinlan, Katharina A; Barlow, Courtenay B et al. (2012) Motor neuron rescue in spinal muscular atrophy mice demonstrates that sensory-motor defects are a consequence, not a cause, of motor neuron dysfunction. J Neurosci 32:3818-29
Frigon, Alain; Hurteau, Marie-France; Johnson, Michael D et al. (2012) Synchronous and asynchronous electrically evoked motor activities during wind-up stimulation are differentially modulated following an acute spinal transection. J Neurophysiol 108:3322-32
Manuel, Marin; Marin, Manuel; Heckman, C J (2012) Simultaneous intracellular recording of a lumbar motoneuron and the force produced by its motor unit in the adult mouse in vivo. J Vis Exp :e4312
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

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