Abstract

BackgroundXenon has minimal haemodynamic side effects when compared to volatile or intravenous anaesthetics. Moreover, in in vitro and in animal experiments, xenon has been demonstrated to convey cardio- and neuroprotective effects. Neuroprotection could be advantageous in paediatric anaesthesia as there is growing concern, based on both laboratory studies and retrospective human clinical studies, that anaesthetics may trigger an injury in the developing brain, resulting in long-lasting neurodevelopmental consequences. Furthermore, xenon-mediated neuroprotection could help to prevent emergence delirium/agitation. Altogether, the beneficial haemodynamic profile combined with its putative organ-protective properties could render xenon an attractive option for anaesthesia of children undergoing cardiac catheterization.Methods/DesignIn a phase-II, mono-centre, prospective, single-blind, randomised, controlled study, we will test the hypothesis that the administration of 50% xenon as an adjuvant to general anaesthesia with sevoflurane in children undergoing elective cardiac catheterization is safe and feasible. Secondary aims include the evaluation of haemodynamic parameters during and after the procedure, emergence characteristics, and the analysis of peri-operative neuro-cognitive function.A total of 40 children ages 4 to 12 years will be recruited and randomised into two study groups, receiving either a combination of sevoflurane and xenon or sevoflurane alone.DiscussionChildren undergoing diagnostic or interventional cardiac catheterization are a vulnerable patient population, one particularly at risk for intra-procedural haemodynamic instability. Xenon provides remarkable haemodynamic stability and potentially has cardio- and neuroprotective properties. Unfortunately, evidence is scarce on the use of xenon in the paediatric population. Our pilot study will therefore deliver important data required for prospective future clinical trials.Trial registrationEudraCT: 2014-002510-23 (5 September 2014)

Highlights

  • Xenon has minimal haemodynamic side effects when compared to volatile or intravenous anaesthetics

  • Evidence is scarce on the use of xenon in the paediatric population

  • Our pilot study will deliver important data required for prospective future clinical trials

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Summary

Introduction

Xenon has minimal haemodynamic side effects when compared to volatile or intravenous anaesthetics. In in vitro and in animal experiments, xenon has been demonstrated to convey cardio- and neuroprotective effects. The first use of xenon for anaesthesia in humans was performed by Cullen and Gross in 1951 [2,3]. Xenon is described as having many of the characteristics of an ideal inhalational anaesthetic agent. It is non-flammable, non-explosive, non-toxic, devoid of teratogenic effects and does not contribute to the greenhouse effect. Xenon affects haemodynamics, myocardial performance and the neurohumoral system less than other anaesthetic agents [4]

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