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新生儿、婴儿及儿童的抗菌治疗

Antimicrobial therapy in neonates, infants and children.

作者信息

Brown R D, Campoli-Richards D M

机构信息

Department of Pharmacology and Therapeutics, School of Medicine, Louisiana State University Medical Center, Shreveport.

出版信息

Clin Pharmacokinet. 1989;17 Suppl 1:105-15. doi: 10.2165/00003088-198900171-00008.

DOI:10.2165/00003088-198900171-00008
PMID:2692934
Abstract

Many antimicrobial medications may be administered to paediatric patients with a degree of impunity because they are relatively non-toxic and have a wide therapeutic margin. However, because of different pharmacokinetics from those in adults, the potential for toxicity exists with the use of some of these agents. Drug absorption in paediatric patients, either orally or parenterally, is generally similar to that in adults, except among neonates and, particularly, premature neonates. Similarly, in neonates, drug distribution is altered, plasma protein binding is decreased and hepatic metabolism and renal excretory capacity are limited by physiological immaturity. Thus, in neonates, only drugs that have pharmacokinetically derived dosage schedules should be used, and therapeutic monitoring of plasma drug concentrations is recommended during therapy with aminoglycosides, vancomycin and chloramphenicol. In older infants and children, the pharmacokinetics of antimicrobial drugs generally approximate those in adults, and recommended dosages have been determined relative to bodyweight. Therapeutic monitoring of plasma drug concentrations may be important in certain patients, such as those with major organ failure, and may be useful in cases of suspected noncompliance. Additional pharmacokinetic considerations concerning antimicrobial medication and paediatric patients are the extent to which drug therapy penetrates the cerebrospinal fluid in meningitis, and the potential for and implications of exposure of infants to antimicrobial medications excreted in breast milk.

摘要

许多抗菌药物可以施用于儿科患者而不会造成太大危害,因为它们相对无毒且治疗窗较宽。然而,由于儿科患者的药代动力学与成人不同,使用某些此类药物时存在毒性风险。儿科患者口服或胃肠外给药的药物吸收情况通常与成人相似,但新生儿尤其是早产儿除外。同样,新生儿的药物分布会发生改变,血浆蛋白结合率降低,肝脏代谢和肾脏排泄能力因生理不成熟而受限。因此,在新生儿中,应仅使用具有根据药代动力学得出的给药方案的药物,并且在使用氨基糖苷类、万古霉素和氯霉素治疗期间建议监测血浆药物浓度。在较大的婴儿和儿童中,抗菌药物的药代动力学通常与成人相近,推荐剂量已根据体重确定。血浆药物浓度的治疗监测在某些患者(如患有主要器官功能衰竭的患者)中可能很重要,并且在怀疑不依从的情况下可能有用。关于抗菌药物与儿科患者的其他药代动力学考虑因素包括药物治疗在脑膜炎中穿透脑脊液的程度,以及婴儿接触母乳中排泄的抗菌药物的可能性及其影响。

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