Significantly Improved Pharmacokinetics Enhances In Vivo Efficacy of APX001 against Echinocandin- and Multidrug-Resistant Candida Isolates in a Mouse Model of Invasive Candidiasis.

Yanan Zhao,Steven Park,Annie Lee,Karen Joy Shaw,Robert S Mansbach,Min Hee Lee,David S Perlin,Padmaja Paderu,Cristina Jimenez-Ortigosa

doi:10.1128/aac.00425-18

Abstract

APX001 is a first-in-class, intravenous and orally available, broad-spectrum antifungal agent in clinical development for the treatment of life-threatening invasive fungal infections. The half-life of APX001A, the active moiety of APX001, is significantly shorter in mice than in humans (1.4 to 2.75 h in mice versus 2 to 2.5 days in humans), making the exploration of efficacy in mouse models difficult. After pretreatment with 1-aminobenzotriazole (ABT), a nonspecific cytochrome P450 inhibitor, greatly increased plasma APX001A exposure was observed in mice of different strains and of both genders. As a consequence, 26 mg/kg APX001 plus ABT sterilized kidneys in mice infected with Candida albicans, while APX001 alone at the same dose resulted in a modest burden reduction of only 0.2 log10 CFU/g, relative to the vehicle control. In the presence of ABT, 2 days of once-daily dosing with APX001 at 26 mg/kg also demonstrated significant in vivo efficacy in the treatment of Candida glabrata infections in mice. Potent kidney burden reduction was achieved in mice infected with susceptible, echinocandin-resistant, or multidrug-resistant strains. In contrast, the standard of care (micafungin) was ineffective in treating infections caused by the resistant C. glabrata isolates.

Highlights

APX001 is a first-in-class, intravenous and orally available, broadspectrum antifungal agent in clinical development for the treatment of lifethreatening invasive fungal infections
The physiochemical properties of ABT make it very helpful as a tool to increase the exposure of coadministered molecules for in vivo studies. The aim of this proof-of-concept study was to evaluate the PK properties and in vivo efficacy of APX001 with greater sustained drug exposure in mice, in the presence of ABT, against infections caused by Candida albicans and Candida glabrata, including echinocandin-resistant (ER) and multidrugresistant (MDR) isolates
APX001A was highly active against all Candida isolates included in this study, with MIC values comparable to or lower than those of other tested antifungals

Summary

Introduction

APX001 is a first-in-class, intravenous and orally available, broadspectrum antifungal agent in clinical development for the treatment of lifethreatening invasive fungal infections. Mouse candidiasis models have historically been used for antifungal drug discovery and development, because data derived from mouse studies are deemed to provide valuable insights relevant to clinical responses Such a marked PK difference in half-lives between humans and mice is likely a result of drug metabolism differences in these two mammalian species. The physiochemical properties of ABT make it very helpful as a tool to increase the exposure of coadministered molecules for in vivo studies The aim of this proof-of-concept study was to evaluate the PK properties and in vivo efficacy of APX001 with greater sustained drug exposure in mice, in the presence of ABT, against infections caused by Candida albicans and Candida glabrata, including echinocandin-resistant (ER) and multidrugresistant (MDR) isolates

Methods

Results

Conclusion