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一线及世卫组织 A 组抗结核药物是否需要进行系统的治疗药物监测?

Has the Time Come for Systematic Therapeutic Drug Monitoring of First-Line and WHO Group A Antituberculosis Drugs?

机构信息

Univ Rennes, CHU Rennes, Inserm, EHESP, Irset (Institut de recherche en santé, environnement et travail); and.

Univ Rennes, CHU Rennes, Inserm, CIC 1414 (Centre d'Investigation Clinique de Rennes), Rennes, France .

出版信息

Ther Drug Monit. 2022 Feb 1;44(1):133-137. doi: 10.1097/FTD.0000000000000948.

Abstract

Tuberculosis (TB) is a major global health issue, with approximately 10 million people being infected each year, and is the leading cause of mortality from infectious disease, with 1.5 million deaths a year. Optimal TB treatment requires a combination of drugs for an adequate treatment duration owing to persistent organisms, hardly accessible infection sites, and a high risk of resistance selection. Long-term therapy increases the risk of patients' loss of adherence, adverse drug reactions, and drug-drug interactions, potentially leading to treatment failure. The high interpatient variability of TB drug exposure is another point eliciting interest in therapeutic drug monitoring (TDM) to optimize treatment. Studies reporting clinically relevant exposure thresholds, which might be proposed as targets toward treatment personalization, are discussed. Practical TDM strategies have also been reported to circumvent issues related to delayed drug absorption and the need for multiple samples when evaluating the area under the curve of drug concentrations. The need for treatment individualization is further emphasized because of the development of multidrug-resistant TB or extensively drug-resistant TB. Finally, the willingness to shorten the treatment duration while maintaining success is also a driver for ensuring adequate exposure to TB drugs with TDM. The aim of the present review was to underline the role of TDM in drug-susceptible TB and World Health Organization group A TB drugs.

摘要

结核病(TB)是一个重大的全球卫生问题,每年约有 1000 万人感染,是传染病死亡的主要原因,每年有 150 万人死亡。由于持续存在的病原体、难以到达的感染部位和高耐药风险,最佳的结核病治疗需要联合使用药物进行足够的治疗时间。长期治疗增加了患者失去依从性、药物不良反应和药物相互作用的风险,可能导致治疗失败。TB 药物暴露的个体间高度差异也引起了人们对治疗药物监测(TDM)的兴趣,以优化治疗。讨论了报告具有临床相关性的药物暴露阈值的研究,这些阈值可能被提议作为治疗个体化的目标。还报告了实用的 TDM 策略,以解决与药物吸收延迟和评估药物浓度曲线下面积时需要多个样本相关的问题。由于耐多药结核病或广泛耐药结核病的发展,需要进一步强调个体化治疗的必要性。最后,通过 TDM 确保结核病药物的充分暴露,也有助于缩短治疗时间而不影响疗效。本综述的目的是强调 TDM 在药物敏感结核病和世界卫生组织 A 组结核病药物中的作用。

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