EVIDENCE THAT GLYCINE AND GABA MEDIATE POSTSYNAPTIC INHIBITION OF BULBAR RESPIRATORY NEURONS IN THE CAT

被引:67
作者
HAJI, A [1 ]
TAKEDA, R [1 ]
REMMERS, JE [1 ]
机构
[1] UNIV CALGARY,HLTH SCI CTR,FAC MED,DEPT MED,RESP RES GRP,3330 HOSP DR NW,CALGARY T2N 4N1,ALBERTA,CANADA
关键词
CONTROL OF BREATHING; BICUCULLINE; STRYCHNINE;
D O I
10.1152/jappl.1992.73.6.2333
中图分类号
Q4 [生理学];
学科分类号
071003 ;
摘要
Experiments were carried out on decerebrate cats to identify transsynaptic mediators of spontaneous postsynaptic inhibition of bulbar inspiratory and postinspiratory neurons. Somatic membrane potentials were recorded through the central micropipette of a coaxial multibarreled electrode. Blockers of type A gamma-aminobutyric acid (GABA-A) and glycine receptors were iontophoresed extracellularly from peripheral micropipettes surrounding the central pipette. Effective antagonism was demonstrated by iontophoresis of agonists with antagonists; application of strychnine antagonized the action of glycine but not GABA, and application of bicuculline antagonized the action of GABA but not glycine. In both types of neurons, iontophoresis of either antagonist depolarized the somatic membrane and increased input resistance throughout the respiratory cycle. Bicuculline preferentially depolarized the somatic membrane in both types of neurons during inactive phases. Strychnine increased the firing rate of inspiratory neurons during inspiration despite maintenance of somatic membrane potential at preiontophoresis levels. Tetrodotoxin reduced the effects of iontophoresed bicuculline and strychnine, suggesting that the action of the antagonists required presynaptic axonal conduction. The present results suggest that presynaptic release of both GABA and glycine contributes to tonic postsynaptic inhibition of bulbar respiratory neurons. GABA-A receptors appear to contribute to inhibition during inactive phases in inspiratory and postinspiratory neurons, whereas glycinergic mechanisms appear to contribute to inspiratory inhibition in inspiratory neurons.
引用
收藏
页码:2333 / 2342
页数:10
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