Abstract
Invasive pulmonary Aspergillosis is a leading cause of morbidity and mortality in immunosuppressed patients and treatment outcomes using oral antifungal triazoles remain suboptimal. Here we show that combining topical treatment using PC945, a novel inhaled triazole, with systemic treatment using known triazoles demonstrated synergistic antifungal effects against Aspergillus fumigatus (AF) in an in vitro human alveolus bilayer model and in the lungs of neutropenic immunocompromised mice. Combination treatment with apical PC945 and either basolateral posaconazole or voriconazole resulted in a synergistic interaction with potency improved over either compound as a monotherapy against both azole-susceptible and resistant AF invasion in vitro. Surprisingly there was little, or no synergistic interaction observed when apical and basolateral posaconazole or voriconazole were combined. In addition, repeated prophylactic treatment with PC945, but not posaconazole or voriconazole, showed superior effects to single prophylactic dose, suggesting tissue retention and/or accumulation of PC945. Furthermore, in mice infected with AF intranasally, 83% of animals treated with a combination of intranasal PC945 and oral posaconazole survived until day 7, while little protective effects were observed by either compound alone. Thus, the combination of a highly optimised topical triazole with oral triazoles potentially induces synergistic effects against AF infection.
Highlights
Inhalation and deposition of Aspergillus conidia in the lung is the most common route of infection for patients who contract invasive aspergillosis[1]
Combination treatment with antifungal compounds with different modes of action has been well documented by fungal culture in microplates, we differentiated for the first time the synergistic antifungal effects of different treatment routes for antifungal triazoles
The in vitro A. fumigatus infection model of the human alveolus has been well characterised by Hope et al and other groups[9,11,12,13,14]
Summary
Inhalation and deposition of Aspergillus conidia in the lung is the most common route of infection for patients who contract invasive aspergillosis[1]. To evaluate the effects of antifungal combinations, standard susceptibility testing in microtiter plates is often used. This system does not differentiate topical and systemic treatment. The system consists of two chambers divided by a porous membrane separating an apical layer of alveolar epithelial cells from a basolateral layer of vascular endothelial cells This system allows a topical compound to be administered apically in upper chamber and/or an oral compound basolaterally in lower chamber. In this report we describe the synergistic effects of combined treatment with topical (PC945) and systemic triazoles against penetration of azole-susceptible and resistant A. fumigatus. Of PC945 was investigated and compared with those of posaconazole and voriconazole to discriminate PC945 from known triazoles based on longer cell residency as well as accumulation, and as this is a key component for the prophylactic treatment of immunocompromised patients
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