临床药代动力学-药效学研究在揭示早期和晚期结核预后决定因素中的重要性。

International journal of pharmacokinetics Pub Date : 2017-08-01 Epub Date: 2017-07-12 DOI:10.4155/ipk-2017-0004
Andrew D McCallum, Derek J Sloan
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引用次数: 14

摘要

结核病仍然是全世界发病率和死亡率的主要传染病。目前的抗生素方案是在现代药代动力学-药效学(PK-PD)工具发展之前构建的,是基于对药物敏感和多重耐药结核病的暴露-反应关系的不完全理解。临床前和人群PK数据表明,临床PK- pd研究可以对某些药物进行治疗性药物监测,并修改其他药物的剂量。未来的临床PK- pd挑战包括:结合PK方法来测定所有活性代谢物的游离浓度;选择反映治疗反应的适当早期结果指标;阐明个体间PK变异的遗传因素;对特殊人群(包括儿童)进行有针对性的研究;以及疾病部位PK-PD参数的测量。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The importance of clinical pharmacokinetic-pharmacodynamic studies in unraveling the determinants of early and late tuberculosis outcomes.

The importance of clinical pharmacokinetic-pharmacodynamic studies in unraveling the determinants of early and late tuberculosis outcomes.

The importance of clinical pharmacokinetic-pharmacodynamic studies in unraveling the determinants of early and late tuberculosis outcomes.

Tuberculosis remains a major infectious cause of morbidity and mortality worldwide. Current antibiotic regimens, constructed prior to the development of modern pharmacokinetic-pharmacodynamic (PK-PD) tools, are based on incomplete understanding of exposure-response relationships in drug susceptible and multidrug resistant tuberculosis. Preclinical and population PK data suggest that clinical PK-PD studies may enable therapeutic drug monitoring for some agents and revised dosing for others. Future clinical PK-PD challenges include: incorporation of PK methods to assay free concentrations for all active metabolites; selection of appropriate early outcome measures which reflect therapeutic response; elucidation of genetic contributors to interindividual PK variability; conduct of targeted studies on special populations (including children); and measurement of PK-PD parameters at the site of disease.

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