危重症患者炎症生物标志物与药物药代动力学的关系：范围综述。

The relation between inflammatory biomarkers and drug pharmacokinetics in the critically ill patients: a scoping review.

机构信息

Department of Hospital Pharmacy, Erasmus MC-University Medical Center, Doctor Molewaterplein 40, 3015 GD, Rotterdam, The Netherlands.

Department of Hospital Pharmacy, Xinqiao Hospital, Army Medical University, 183 Xinqiao Street, Shapingba District, Chongqing, 400037, China.

出版信息

Crit Care. 2024 Nov 19;28(1):376. doi: 10.1186/s13054-024-05150-4.

DOI:10.1186/s13054-024-05150-4

PMID:39563441

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11577668/

Abstract

BACKGROUND

The level of inflammation alters drug pharmacokinetics (PK) in critically ill patients. This might compromise treatment efficacy. Understanding the specific effects of inflammation, measured by biomarkers, on drug absorption, distribution, metabolism, and excretion is might help in optimizing dosing strategies.

OBJECTIVES

This review investigates the relationship between inflammatory biomarkers and PK parameters absorption, distribution, metabolism and excretion (ADME) in critically ill patients, providing insight in the complexity of dosing drugs in critically ill patients.

METHOD

Following PRISMA guidelines, we conducted a comprehensive search of Medline, Embase, Web of Science, and Cochrane databases (January 1946-November 2023). Studies examining inflammatory biomarkers, PK parameters, or drug exposure in critically ill patients were included. Records were screened by title, abstract, and full text, with any discrepancies resolved through discussion or consultation with a third reviewer.

RESULTS

Of the 4479 records screened, 31 met our inclusion criteria: 2 on absorption, 7 on distribution, 17 on metabolism, and 6 on excretion. In general, results are only available for a limited number of drugs, and most studies are done only looking at one of the components of ADME. Higher levels of inflammatory biomarkers may increase or decrease drug absorption depending on whether the drug undergoes hepatic first-pass elimination. For drug distribution, inflammation is negatively correlated with drug protein binding capacity, positively correlated with cerebrospinal fluid penetration, and negatively correlated with peritoneal penetration. Metabolizing capacity of most drugs was inversely correlated with inflammatory biomarkers. Regarding excretion, inflammation can lead to reduced drug clearance, except in the neonatal population.

CONCLUSION

Inflammatory biomarkers can offer valuable information regarding altered PK in critically ill patients. Our findings emphasize the need to consider inflammation-driven PK variability when individualizing drug therapy in this setting, at the same time research is limited to certain drugs and needs further research, also including pharmacodynamics.

摘要

背景

炎症水平改变了危重症患者的药物药代动力学（PK）。这可能会影响治疗效果。了解炎症标志物对药物吸收、分布、代谢和排泄（ADME）的具体影响，可能有助于优化给药策略。

目的

本综述调查了炎症标志物与危重症患者 PK 参数吸收、分布、代谢和排泄（ADME）之间的关系，深入了解了在危重症患者中给药的复杂性。

方法

根据 PRISMA 指南，我们对 Medline、Embase、Web of Science 和 Cochrane 数据库（1946 年 1 月至 2023 年 11 月）进行了全面检索。纳入研究检查了炎症标志物、PK 参数或药物暴露在危重症患者中的情况。通过标题、摘要和全文筛选记录，如果存在任何分歧，则通过讨论或咨询第三位审稿人解决。

结果

在筛选的 4479 条记录中，有 31 条符合我们的纳入标准：2 条关于吸收，7 条关于分布，17 条关于代谢，6 条关于排泄。一般来说，结果仅适用于有限数量的药物，并且大多数研究仅研究 ADME 的一个组成部分。较高水平的炎症标志物可能会增加或减少药物吸收，具体取决于药物是否经历肝脏首过消除。对于药物分布，炎症与药物蛋白结合能力呈负相关，与脑脊液穿透呈正相关，与腹膜穿透呈负相关。大多数药物的代谢能力与炎症标志物呈负相关。关于排泄，炎症可导致药物清除率降低，新生儿人群除外。