School of Translational Medicine, The University of Manchester, and Manchester Academic Health Science Centre, National Institute for Health Research Translational Research Facility in Respiratory Medicine, University Hospital of South Manchester National Health Service, Foundation Trust, Manchester, United Kingdom.
Antimicrob Agents Chemother. 2012 Aug;56(8):4146-53. doi: 10.1128/AAC.00141-12. Epub 2012 May 21.
Itraconazole is used for the prevention and treatment of infections caused by Aspergillus fumigatus. An understanding of the pharmacodynamics of itraconazole against wild-type and triazole-resistant strains provides a basis for innovative therapeutic strategies for treatment of infections. An in vitro model of the human alveolus was used to define the pharmacodynamics of itraconazole. Galactomannan was used as a biomarker. The effect of systemic and airway administration of itraconazole was assessed, as was a combination of itraconazole administered to the airway and systemically administered 5FC. Systemically administered itraconazole against the wild type induced a concentration-dependent decline in galactomannan in the alveolar and endothelial compartments. No exposure-response relationships were apparent for the L98H, M220T, or G138C mutant. The administration of itraconazole to the airway resulted in comparable exposure-response relationships to those observed with systemic therapy. This was achieved without detectable concentrations of drug within the endothelial compartment. The airway administration of itraconazole resulted in a definite but submaximal effect in the endothelial compartment against the L98H mutant. The administration of 5FC resulted in a concentration-dependent decline in galactomannan in both the alveolar and endothelial compartments. The combination of airway administration of itraconazole and systemically administered 5FC was additive. Systemic administration of itraconazole is ineffective against Cyp51 mutants. The airway administration of itraconazole is effective for the treatment of wild-type strains and appears to have some activity against the L98H mutants. Combination with other agents, such as 5FC, may enable the attainment of near-maximal antifungal activity.
伊曲康唑用于预防和治疗烟曲霉引起的感染。了解伊曲康唑对野生型和三唑耐药株的药效动力学为治疗感染的创新治疗策略提供了基础。使用人肺泡的体外模型来定义伊曲康唑的药效动力学。半乳甘露聚糖被用作生物标志物。评估了伊曲康唑全身和气道给药的效果,以及气道给予伊曲康唑和全身给予 5FC 的联合用药效果。针对野生型的全身给予伊曲康唑会导致肺泡和内皮隔室中的半乳甘露聚糖浓度依赖性下降。对于 L98H、M220T 或 G138C 突变体,没有明显的暴露-反应关系。气道给予伊曲康唑会导致与全身治疗观察到的类似的暴露-反应关系。这是在没有检测到内皮隔室内药物浓度的情况下实现的。气道给予伊曲康唑会导致内皮隔室中针对 L98H 突变体产生明确但亚最大效应。5FC 的给药会导致肺泡和内皮隔室中的半乳甘露聚糖浓度依赖性下降。气道给予伊曲康唑和全身给予 5FC 的联合使用具有相加作用。全身给予伊曲康唑对 Cyp51 突变体无效。气道给予伊曲康唑对野生型菌株有效,并且似乎对 L98H 突变体具有一定的活性。与其他药物(如 5FC)联合使用可能使获得接近最大的抗真菌活性成为可能。