Blunted response to low oxygen of rat respiratory network after perinatal ethanol exposure: involvement of inhibitory control
Acute ethanol depresses respiration, but little is known about chronic ethanol exposure during gestation and breathing, while the deleterious effects of ethanol on CNS development have been clearly described. In a recent study we demonstrated that pre- and postnatal ethanol exposure induced low minu...
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Veröffentlicht in: | The Journal of physiology 2008-03, Vol.586 (5), p.1413-1427 |
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Zusammenfassung: | Acute ethanol depresses respiration, but little is known about chronic ethanol exposure during gestation and breathing, while
the deleterious effects of ethanol on CNS development have been clearly described. In a recent study we demonstrated that
pre- and postnatal ethanol exposure induced low minute ventilation in juvenile rats. The present study analysed in juvenile
rats the respiratory response to hypoxia in vivo by plethysmography and the phrenic (Phr) nerve response to ischaemia in situ . Glycinergic neurotransmission was assessed in situ with strychnine application and [ 3 H]strychnine binding experiments performed in the medulla. After chronic ethanol exposure, hyperventilation during hypoxia
was blunted in vivo . In situ Phr nerve response to ischaemia was also impaired, while gasping activity occurred earlier and recovery was delayed. Strychnine
applications in situ (0.05â0.5 μ m ) demonstrated a higher sensitivity of expiratory duration in ethanol-exposed animals compared to control animals. Moreover,
[ 3 H]strychnine binding density was increased after ethanol and was associated with higher affinity. Furthermore, 0.2 μ m strychnine in ethanol-exposed animals restored the low basal Phr nerve frequency, but also the Phr nerve response to ischaemia
and the time to recovery, while gasping activity appeared even earlier with a higher frequency. Polycythaemia was present
after ethanol exposure whereas lung and heart weights were not altered. We conclude that chronic ethanol exposure during rat
brain development (i) induced polycythaemia to compensate for low minute ventilation at rest; (ii) impaired the respiratory
network adaptive response to low oxygen because of an increase in central glycinergic tonic inhibitions, and (iii) did not
affect gasping mechanisms. We suggest that ethanol exposure during early life can be a risk factor for the newborn respiratory
adaptive mechanisms to a low oxygen environment. |
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ISSN: | 0022-3751 1469-7793 |
DOI: | 10.1113/jphysiol.2007.147165 |