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Growing up with midazolam in the neonatal and pediatric intensive care

机译:在新生儿和小儿科学重症监护下培养咪达唑仑

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A variety of developmental changes is of influence on the pharmacokinetics and pharmacodynamics of midazolam in neonatal and pediatric intensive care patients. However, dosing regimens in children are based upon rather empirical extrapolations from the dosing regimens in adults. Based on current available studies it appears that with the rising of age, the pharmacokinetics of intravenously administered midazolam alter, resulting in a shorter half-life due to a higher hepatic clearance in older children as compared to newborn. Also, with the rising of age, the pharmacodynamics of intravenously administered midazolam may alter due to a decrease in density of receptors, possibly leading to a decreased clinical response. These findings implicate opposite effects and it is uncertain which of these effects are predominant. In conclusion, there is a large interindividual variability in the response to midazolam in children, which may be caused by differences in pharmacokinetics and pharmacodynamics. Both are subject to considerable developmental changes. It remains remarkable that high-quality evidence to support the use of midazolam for continuous sedation in the neonatal and pediatric intensive care setting is lacking.
机译:各种发育变化对新生儿和儿科密集护理患者中咪达唑仑的药代动力学和药效学的影响。然而,儿童的给药方案基于来自成人的给药方案的相当实证的外推。基于当前可用的研究,似乎随着年龄的增加,静脉内施用的咪达唑仑的药代动力学改变,导致年龄较短的半衰期由于新生儿的肝脏肝脏肝脏较高。此外,随着年龄的上升,由于受体密度降低,静脉内施用的MidazoLam的药效学可能会改变,可能导致临床反应降低。这些发现涉及相反的效果,并且不确定这些效果中的哪一个是主要的。总之,对儿童中咪达唑仑的反应存在大的易变异性,这可能是由药代动力学和药效学的差异引起的。两者都受到相当大的发展变化。缺乏缺乏高质量证据,以支持咪达唑仑在新生儿和儿科重症监护环境中使用咪达唑仑的高质量证据。

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