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Posaconazole Exposure-Response Relationship: Evaluating the Utility of Therapeutic Drug Monitoring

机译:泊沙康唑的暴露-反应关系:评估治疗药物监测的效用

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摘要

Posaconazole has become an important part of the antifungal armamentarium in the prophylaxis and salvage treatment of invasive fungal infections (IFIs). Structurally related to itraconazole, posaconazole displays low oral bioavailability due to poor solubility, with significant drug interactions and gastrointestinal disease also contributing to the generally low posaconazole plasma concentrations observed in patients. While therapeutic drug monitoring (TDM) of plasma concentrations is widely accepted for other triazole antifungal agents such as voriconazole, the utility of TDM for posaconazole is controversial due to debate over the relationship between posaconazole exposure in plasma and clinical response to therapy. This review examines the available evidence for a relationship between plasma concentration and clinical efficacy for posaconazole, as well as evaluating the utility of TDM and providing provisional target concentrations for posaconazole therapy. Increasing evidence supports an exposure-response relationship for plasma posaconazole concentrations for prophylaxis and treatment of IFIs; a clear relationship has not been identified between posaconazole concentration and toxicity. Intracellular and intrapulmonary concentrations have been studied for posaconazole but have not been correlated to clinical outcomes. In view of the high mortality and cost associated with the treatment of IFIs, increasing evidence of an exposure-response relationship for posaconazole efficacy in the prevention and treatment of IFIs, and the common finding of low posaconazole concentrations in patients, TDM for posaconazole is likely to be of significant clinical utility. In patients with subtherapeutic posaconazole concentrations, increased dose frequency, administration with high-fat meals, and withdrawal of interacting medications from therapy are useful strategies to improve systemic absorption.
机译:在预防和挽救侵入性真菌感染(IFIs)方面,泊沙康唑已成为抗真菌药库的重要组成部分。在结构上与伊曲康唑有关,泊沙康唑由于溶解度差而显示出较低的口服生物利用度,与药物的显着相互作用和胃肠道疾病也导致患者体内普遍观察到的泊沙康唑血浆浓度较低。虽然其他三唑类抗真菌药(如伏立康唑)的血浆浓度治疗药物监测(TDM)已被广泛接受,但由于对血浆中泊沙康唑暴露与对治疗的临床反应之间的关系存在争议,因此TDM在泊沙康唑中的应用存在争议。这篇综述检查了血浆浓度与泊沙康唑临床疗效之间关系的可用证据,并评估了TDM的效用并提供了泊沙康唑治疗的临时目标浓度。越来越多的证据支持血浆泊沙康唑浓度与暴露-反应的关系,以预防和治疗IFI;泊沙康唑的浓度与毒性之间没有明确的关系。已经研究了泊沙康唑的细胞内和肺内浓度,但与临床结果无关。鉴于与IFI的治疗相关的高死亡率和高成本,越来越多的证据表明泊沙康唑在IFI的预防和治疗中具有疗效-暴露-反应关系,并且患者中泊沙康唑浓度低的普遍发现,可能使用TDM治疗泊沙康唑具有重要的临床用途。在亚治疗型泊沙康唑浓度较高的患者中,增加用药频率,高脂饮食和停用相互作用药物是改善全身吸收的有用策略。

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