4.6 Article

A neurosteroid analogue with T-type calcium channel blocking properties is an effective hypnotic, but is not harmful to neonatal rat brain

期刊

BRITISH JOURNAL OF ANAESTHESIA
卷 120, 期 4, 页码 768-778

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ELSEVIER SCI LTD
DOI: 10.1016/j.bja.2017.12.039

关键词

calcium channels; developmental neurotoxicity; neurosteroid

资金

  1. Department of Anesthesiology at the University of Colorado Anschutz Medical campus
  2. National Institute of Health [GM102525, R0144517, R0144517-S, R01 GM118197, R21 HD080281]
  3. National Institute of Health (March of Dimes National Award, USA)
  4. University of Colorado Medicine Endowment
  5. Taylor Family Institute for Innovative Psychiatric Research

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Background: More than 4 million children are exposed annually to sedatives and general anaesthetics (GAs) in the USA alone. Recent data suggest that common GAs can be detrimental to brain development causing neurodegeneration and long-term cognitive impairments. Challenged by a recent US Food and Drug Administration (FDA) warning about potentially neurotoxic effects of GAs in children, there is an urgent need to develop safer GAs. Methods: Postnatal Day 7 (P7) rat pups of both sexes were exposed to six (repeated every 2 h) injections of equipotent hypnotic doses of ketamine or the neuroactive steroid (3 beta, 5 beta, 17 beta)-3-hydroxyandrostane-17-carbonitrile (3 beta-OH) for 12 h. Loss of righting reflex was used to assess hypnotic properties and therapeutic index; quantitative caspase-3 immunohistochemistry was used to assess developmental neuroapoptosis; patch-clamp recordings in acute brain slices were used to assess the effects of 3 beta-OH on neuronal excitability and synaptic transmission. Cognitive abilities of rats exposed to ketamine, 3 beta-OH, or vehicle at P7 were assessed in young adulthood using the radial arm maze. Results: The neuroactive steroid 3 beta-OH has a therapeutic index similar to ketamine, a commonly used clinical GA. We report that 3 beta-OH is safe and, unlike ketamine, does not cause neuroapoptosis or impair cognitive development when administered to P7 rat pups. Interestingly, 3 beta-OH blocks T-type calcium channels and presynaptically dampens synaptic transmission at hypnotically-relevant brain concentrations, but it lacks a direct effect on g-aminobutyric acid A or glutamate-gated ion channels. Conclusions: The neurosteroid 3 beta-OH is a relatively safe hypnotic that warrants further consideration for paediatric anaesthesia.

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