Impact of CYP2C19 Genotype and Drug Interactions on Voriconazole Plasma Concentrations: A Spain Pharmacogenetic‐Pharmacokinetic Prospective Multicenter Study

伏立康唑 CYP2C19型 医学 治疗药物监测 药代动力学 内科学 药理学 基因型 不利影响 药物遗传学 槽水位 CYP2D6型 胃肠病学 药效学 CYP3A4型 CYP3A5 药品 药物相互作用 基因分型 加药 人口 细胞色素P450 生物 抗真菌 基因 新陈代谢 生物化学 皮肤病科 他克莫司 移植
作者
Sara Blanco‐Dorado,Olalla Maroñas,Ana Latorre‐Pellicer,María Teresa Rodríguez Jato,Ana López‐Vizcaíno,Aurea Gómez Márquez,Belén Bardán García,Dolores Belles Medall,Gema Barbeito Castiñeiras,María Luisa Pérez del Molino Bernal,Manuel Campos‐Toimil,Francisco J. Otero-Espinar,Andrés Blanco Hortas,Goretti Duran,Irene Zarra-Ferro,Ángel Carracedo,María Jesús Lamas,Anxo Fernández‐Ferreiro
出处
期刊:Pharmacotherapy [Wiley]
卷期号:40 (1): 17-25 被引量:14
标识
DOI:10.1002/phar.2351
摘要

Background Voriconazole, a first‐line agent for the treatment of invasive fungal infections, is mainly metabolized by cytochrome P450 (CYP) 2C19. A significant portion of patients fail to achieve therapeutic voriconazole trough concentrations, with a consequently increased risk of therapeutic failure. Objective To show the association between subtherapeutic voriconazole concentrations and factors affecting voriconazole pharmacokinetics: CYP2C19 genotype and drug–drug interactions. Methods Adults receiving voriconazole for antifungal treatment or prophylaxis were included in a multicenter prospective study conducted in Spain. The prevalence of subtherapeutic voriconazole troughs was analyzed in the rapid metabolizer and ultra‐rapid metabolizer patients (RMs and UMs, respectively), and compared with the rest of the patients. The relationship between voriconazole concentration, CYP2C19 phenotype, adverse events (AEs), and drug–drug interactions was also assessed. Results In this study 78 patients were included with a wide variability in voriconazole plasma levels with only 44.8% of patients attaining trough concentrations within the therapeutic range of 1 and 5.5 µg/ml. The allele frequency of *17 variant was found to be 29.5%. Compared with patients with other phenotypes, RMs and UMs had a lower voriconazole plasma concentration (RM/UM: 1.85 ± 0.24 µg/ml vs other phenotypes: 2.36 ± 0.26 µg/ml). Adverse events were more common in patients with higher voriconazole concentrations (p<0.05). No association between voriconazole trough concentration and other factors (age, weight, route of administration, and concomitant administration of enzyme inducer, enzyme inhibitor, glucocorticoids, or proton pump inhibitors) was found. Conclusion These results suggest the potential clinical utility of using CYP2C19 genotype‐guided voriconazole dosing to achieve concentrations in the therapeutic range in the early course of therapy. Larger studies are needed to confirm the impact of pharmacogenetics on voriconazole pharmacokinetics.

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