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Equipotent subanesthetic concentrations of sevoflurane and xenon preventing cold-stimulated vocalization of neonatal rats

机译:七氟醚和氙的等级粒度浓度,防止新生大鼠的冷刺激声

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摘要

Methods: Forty-eight Wistar rats (Charles River Laboratories, Kent, United Kingdom) on postnatal day 9 were randomized to eight concentrations of inhaled anesthetics: isoflurane, sevoflurane, or xenon. Exposure was closely monitored in individual metal-based chambers resting on a 35°C mat to maintain normothermia. A 25°C mat was used to stimulate vocalization and a sound recording made (1 min, 1 to 100 kHz). Rectal temperature or partial pressure of carbon dioxide and pH of mixed arteriovenous blood were measured immediately after the exposure. Concentration-response models were constructed using logistic regression (dependent variable: vocalization and explanatory variable: concentration). The effects of all other explanatory variables were assessed by inserting them individually into the model.Background: The effects of inhaled anesthetics on the developing brain are studied using neonatal rodents exposed to fractions of minimum alveolar concentration (to avoid cardiorespiratory compromise). However, these fractions cannot be assumed to be equipotent. Xenon's anesthetic and neuroprotective properties warrant investigation in these models. Therefore, equipotent, subanesthetic concentrations of inhaled anesthetics are needed.Results: The effective inhaled concentrations preventing cold-stimulated vocalization in 50 and 95% of neonatal rats (EiC50 and EiC95) on postnatal day 9 were 0.46 and 0.89% sevoflurane and 20.15 and 34.81% xenon, respectively. The effect on the EiC50 of all other explanatory variables, including duration, was minimal. Stability of EiC50 isoflurane was not achieved over three durations (40, 80, and 120 min exposure). Partial pressure of carbon dioxide and pH in mixed arteriovenous blood appeared normal.Conclusions: The authors report equipotent subanesthetic concentrations of sevoflurane and xenon in neonatal rats with preserved cardiopulmonary function. This may be useful in designing neonatal rodent models of anesthesia.
机译:方法:第9天的四十八只Wistar大鼠(Charles River Laboratories,Kent,United Kingdom)被随机分配到八种浓度的吸入麻醉剂:异氟醚,七氟醚或氙。在35°C垫上靠在35°C的垫子上以维持常温,在静止的基于金属的腔室中密切监测暴露。 25°C垫用于刺激发声,发出声音记录(1分钟,1至100 kHz)。暴露后立即测量二氧化碳的直肠温度或二氧化碳的分压和混合动血管血液的pH值。使用逻辑回归构建浓度 - 响应模型(从属变量:发声和解释变量:浓度)。通过单独插入模型中的所有其他解释变量对所有其他解释性变量的影响然而,这些分数不能被认为是等待的。氙气的麻醉和神经保护性能在这些模型中调查。因此,需要等渗,次间质浓度的吸入麻醉剂。结果:预防50和95%的新生大鼠90和95%的新生大鼠90和95%的新生大鼠(Eic50和Eic95)的有效吸入浓度为0.46和0.89%七氟醚和20.15和34.81分别为氙。对所有其他解释变量的EIC50的影响,包括持续时间最小。在三个持续时间(40,80和120分钟暴露)上未实现EIC50异氟醚的稳定性。二氧化碳的分压和混合动静脉血液中的pH值出现正常。结论:作者报告了具有保存的心肺功能的新生大鼠七氟醚和氙的等渗次生浓度。这对于设计麻醉的新生儿啮齿动物模型可能是有用的。

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  • 来源
    《Anesthesiology》 |2014年第6期|共9页
  • 作者单位

    School of Clinical Sciences University of Bristol St. Michael's Hospital Southwell StreetBristol;

    School of Clinical Sciences University of Bristol St. Michael's Hospital Southwell StreetBristol;

    School of Clinical Sciences University of Bristol St. Michael's Hospital Southwell StreetBristol;

    School of Clinical Sciences University of Bristol St. Michael's Hospital Southwell StreetBristol;

    School of Clinical Sciences University of Bristol St. Michael's Hospital Southwell StreetBristol;

    Department of Physiology Institute of Basic Medical Sciences University of OsloOslo Norway;

    Department of Anaesthesia Swansea University College of Medicine United Kingdom;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 麻醉学;
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