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Department of Physiology, McGill University, Montreal, Quebec, Canada H3G 1Y6
The
objective of this study was to evaluate effects of baclofen, a
-aminobutyric acid type B
(GABAB) receptor agonist, injected into the nucleus of the solitary tract, on the Hering-Breuer
inspiratory-inhibitory (TI-inhibitory) and deflation
reflexes in urethan-anesthetized adult Wistar rats
(n = 7). The
TI-inhibitory reflex was
estimated from changes in peak amplitude of the integrated
diaphragmatic electromyogram and inspiratory time
(TI) provoked by airway
occlusion at end expiration. The deflation reflex was evaluated from
changes in TI and expiration
(TE) of the first two breaths
(TI-1,
TE-1 and
TI-2,
TE-2) immediately after a
decrease in tracheal pressure (Ptr). Under control conditions, airway
occlusion at end-TE prolonged TI (66 ± 5%; mean ± SE)
and the following TE (54 ± 11%). Decreases in Ptr, from
2 to
5
cmH2O, evoked an increase in
TI and shortening of
TE of both breaths. Both effects
were Ptr dependent, and TI-1 and
TE-1 differed from
TI-2 and
TE-2, suggesting a rapid
adaptation to the stimulus. At Ptr of
5
cmH2O,
TI-1 and
TI-2 increased by 30 ± 2 and
43 ± 6%, respectively, and
TE-1 and
TE-2 decreased by 53 ± 4 and
33 ± 7%, respectively. During unloaded breathing, 60 pmol baclofen
prolonged TI by 120 ± 11%
and left TE unaffected. Baclofen
abolished vagally mediated changes in
TE. On the other hand, the
TI increases caused by either
airway occlusion (24 ± 8%) or Ptr of
5
cmH2O
(TI-1; 16 ± 5%) were still
significant, but TI-1 and
TI-2 were not different. A
GABAB receptor antagonist, CGP-35348 (2.8 nmol), reversed
these effects of baclofen. These results imply that stimulation of
GABAB receptors attenuates but does abolish vagally mediated control of
TI. The difference in effects of
baclofen on the central and vagal control of
TI and TE suggests different
distribution of GABAB receptors in
neuronal networks controlling each of these respiratory phases.
airway occlusion; nucleus of the solitary tract; CGP-35348
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