新生儿抗生素药代动力学。

A L Smith
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引用次数: 0

摘要

非代谢极性抗生素的分布体积大致相当于细胞外液区,可由肾脏清除。因此,当给予恒定剂量时,ECF的体积影响Cmax的大小。肾小球滤过率的变化,或在β -内酰胺肾血浆流量的情况下,改变药物从体内清除的速度。代谢抗生素的药代动力学是复杂的;药物前药代动力学不仅影响观察到的活性药物的血清浓度,而且肝血流和胆道血流速率也影响这些抗生素(即氯霉素)从血清中去除的速度。在这些情况下,一般剂量指南几乎不可能适用于新生儿;监测血清浓度是必须的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Antibiotic pharmacokinetics in newborns.

Non-metabolized polar antibiotics have a volume of distribution roughly equivalent to the extracellular fluid compartment and are cleared by the kidney. The volume of the ECF, therefore, affects the magnitude of Cmax when a constant dose is administered. Variations in glomerular filtration rate, or in the case of beta-lactams renal plasma flow, vary the rate at which the drug is cleared from the body. The pharmacokinetics of metabolizable antibiotics is complex; not only does prodrug pharmacokinetics affect the observed serum concentration of the active agent, but hepatic blood flow and biliary flow rate affect the rate at which such antibiotics (i.e., chloramphenicol) are removed from the serum. In these, general dosage guidelines are almost impossible in newborns; monitoring the serum concentrations is mandatory.

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