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The Journal of Neuroscience, March 15, 1999, 19(6):2368-2380
Concurrent Inhibition and Excitation of Phrenic Motoneurons
during Inspiration: Phase-Specific Control of Excitability
M. A.
Parkis1,
X.-W.
Dong2,
J. L.
Feldman3, and
G. D.
Funk1
1 Department of Physiology, Faculty of Medicine and
Health Sciences, University of Auckland, Auckland, New Zealand,
2 Schering-Plow Research Institute, CNS/CV Research,
Kenilworth, New Jersey 07033, and 3 Systems Neurobiology
Laboratory, Departments of Neurobiology and Physiological Science,
University of California Los Angeles, Los Angeles, California
90095-1763
The movements that define behavior are controlled by motoneuron
output, which depends on the excitability of motoneurons and the
synaptic inputs they receive. Modulation of motoneuron excitability takes place over many time scales. To determine whether motoneuron excitability is specifically modulated during the active versus the
quiescent phase of rhythmic behavior, we compared the input-output properties of phrenic motoneurons (PMNs) during inspiratory and expiratory phases of respiration.
In neonatal rat brainstem-spinal cord preparations that generate
rhythmic respiratory motor outflow, we blocked excitatory inspiratory
synaptic drive to PMNs and then examined their phase-dependent responses to superthreshold current pulses. Pulses during inspiration elicited fewer action potentials compared with identical pulses during
expiration. This reduced excitability arose from an inspiratory-phase inhibitory input that hyperpolarized PMNs in the absence of excitatory inspiratory inputs. Local application of bicuculline blocked this inhibition as well as the difference between inspiratory and expiratory firing. Correspondingly, bicuculline locally applied to the midcervical spinal cord enhanced fourth cervical nerve (C4) inspiratory burst amplitude. Strychnine had no effect on C4 output. Nicotinic receptor antagonists neither potentiated C4 output nor blocked its potentiation by bicuculline, further indicating that the inhibition is not from
recurrent inhibitory pathways. We conclude that it is bulbospinal in origin.
These data demonstrate that rapid changes in motoneuron excitability
occur during behavior and suggest that integration of overlapping,
opposing synaptic inputs to motoneurons is important in controlling
motor outflow. Modulation of phasic inhibition may represent a means
for regulating the transfer function of PMNs to suit behavioral demands.
Key words:
phrenic motoneuron; brainstem; spinal cord; respiration; GABA; neonatal rat
Copyright © 1999 Society for Neuroscience 0270-6474/99/1962368-13$05.00/0
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