Covert actions of epidural stimulation on spinal locomotor circuits.
D Leonardo Garcia-RamirezJenna R McGrathNgoc T HaJaimena H WheelSebastian J AtocheLihua YaoNicholas J StachowskiSimon F GiszterKimberly J DoughertyPublished in: bioRxiv : the preprint server for biology (2024)
Spinal circuitry produces the rhythm and patterning of locomotion. However, both descending and sensory inputs are required to initiate and adapt locomotion to the environment. Spinal cord injury (SCI) disrupts descending controls of the spinal cord, producing paralysis. Epidural stimulation (ES) is a promising clinical therapy for motor control recovery and is capable of reactivating the lumbar spinal locomotor networks, yet little is known about the effects of ES on locomotor neurons. Previously, we found that both sensory afferent pathways and serotonin exert mixed excitatory and inhibitory actions on lumbar interneurons involved in the generation of the locomotor rhythm, identified by the transcription factor Shox2. However, after chronic complete SCI, sensory afferent inputs to Shox2 interneurons become almost exclusively excitatory and Shox2 interneurons are supersensitive to serotonin. Here, we investigated the effects of ES on these SCI-induced changes. Inhibitory input from sensory pathways to Shox2 interneurons was maintained and serotonin supersensitivity was not observed in SCI mice that received daily sub-motor threshold ES. Interestingly, the effects of ES were maintained for at least three weeks after the ES was discontinued. In contrast, the effects of ES were not observed in Shox2 interneurons from mice that received ES after the establishment of the SCI-induced changes. Our results demonstrate mechanistic actions of ES at the level of identified spinal locomotor circuit neurons and the effectiveness of early treatment with ES on preservation of spinal locomotor circuitry after SCI, suggesting possible therapeutic benefits prior to the onset of motor rehabilitation.
Keyphrases
- spinal cord injury
- spinal cord
- neuropathic pain
- transcription factor
- randomized controlled trial
- systematic review
- atrial fibrillation
- magnetic resonance
- physical activity
- computed tomography
- metabolic syndrome
- oxidative stress
- blood pressure
- diabetic rats
- mass spectrometry
- high resolution
- skeletal muscle
- insulin resistance
- prefrontal cortex