儿科万古霉素模型引导精准用药的临床应用与挑战

doi:10.12372/jcp.2026.25e1110

摘要/Abstract

摘要：

万古霉素是治疗革兰阳性菌感染，尤其是耐甲氧西林金黄色葡萄球菌感染的关键糖肽类抗生素。然而，儿科患者显著的药代动力学异质性导致传统给药方案较难平衡儿童患者的疗效与肾毒性风险。模型引导的精准用药（MIPD）策略通过整合定量药理学模型（如PPK、PBPK及机器学习模型）与患者个体数据，为实现基于24小时药时曲线下面积与最低抑菌浓度比值（AUC_0-24h/MIC）的个体化治疗提供了新途径。MIPD策略相较于传统治疗药物监测（TDM），能显著提升药代动力学/药效学靶标的达标率，尤其在新生儿和重症患者中可缩短达标时间，同时有效降低肾毒性风险。本文综述了MIPD策略在新生儿、重症患儿及特殊疾病儿童中指导万古霉素应用的临床价值，以期为临床精准用药提供参考。

关键词: 模型引导精准用药, 万古霉素, 群体药代动力学, 有效性, 安全性, 儿科

Abstract:

Vancomycin is a key glycopeptide antibiotic for the treatment of Gram-positive bacterial infections, particularly those caused by methicillin-resistant Staphylococcus aureus (MRSA). However, significant pharmacokinetic (PK) heterogeneity in pediatric patients makes it difficult for traditional dosing regimens to balance efficacy and nephrotoxicity risk. Model-Informed precision dosing (MIPD) strategies provide a novel approach for individualized, AUC_0-24h/MIC-guided therapy by integrating quantitative pharmacological models (such as PPK, PBPK, and machine learning models) with individual patient data. Compared to conventional TDM, MIPD strategies significantly enhance the attainment rate of pharmacokinetic/pharmacodynamic (PK/PD) target concentrations (e.g., AUC), shorten the time to target attainment, especially in neonates and critically ill patients, and effectively reduce the risk of nephrotoxicity. This review summarizes the clinical value of MIPD-guided vancomycin application in neonates, critically ill children, and children with special disease conditions, intending to provide a reference for clinical practice.

Key words: model-informed precision dosing, vancomycin, population pharmacokinetics, efficacy, safety, pediatrics

中图分类号:

姚昀璐, 许海鑫, 刘昕竹, 陈霁晖, 卜书红. 儿科万古霉素模型引导精准用药的临床应用与挑战[J]. 临床儿科杂志, 2026, 44(1): 84-90.

YAO Yunlu, XU Haixin, LIU Xinzhu, CHEN Jihui, BU Shuhong. Clinical practice and challenges of model-informed precision dosing with vancomycin in pediatrics[J]. Journal of Clinical Pediatrics, 2026, 44(1): 84-90.

图/表 1

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模型类型	侧重人群与应用场景	主要优势	主要局限与挑战
群体药代动力学（PPK）	常规患者群体：基于已知协变量（如年龄、肾功能）进行TDM和剂量个体化	方法学成熟，监管认可度高；善于量化个体间差异；适用于临床稀疏采样数据	外推受限：难以准确外推至模型开发未覆盖的特殊人群；机制描述相对简化
生理药代动力学（PBPK）	特殊人群：儿童、孕妇、器官损伤患者等（数据稀缺人群）；预测复杂相互作用的影响	机制驱动：生物学基础强，可解释性高；强大的跨人群（如成人至儿童）外推能力	构建复杂：所需生理及药物参数众多且获取困难；参数不确定性可能累积
人工智能（AI）	大数据/异构数据情景：整合EHR、组学等多源数据；预测复杂终点（疗效/毒性）	数据驱动：强大的非线性模式识别能力；能处理高维复杂数据；模型可动态学习	可解释性差（黑箱问题）；高度依赖训练数据质量，易过拟合；监管验证标准有待完善