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Research Article

Pharmacodynamics of the Orotomides against Aspergillus fumigatus: New Opportunities for Treatment of Multidrug-Resistant Fungal Disease

William W. Hope, Laura McEntee, Joanne Livermore, Sarah Whalley, Adam Johnson, Nicola Farrington, Ruwanthi Kolamunnage-Dona, Julie Schwartz, Anthony Kennedy, Derek Law, Michael Birch, John H. Rex
Robert A. Bonomo, Editor
William W. Hope
a Antimicrobial Pharmacodynamics and Therapeutics, University of Liverpool, Liverpool, United Kingdom
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Laura McEntee
a Antimicrobial Pharmacodynamics and Therapeutics, University of Liverpool, Liverpool, United Kingdom
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Joanne Livermore
a Antimicrobial Pharmacodynamics and Therapeutics, University of Liverpool, Liverpool, United Kingdom
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Sarah Whalley
a Antimicrobial Pharmacodynamics and Therapeutics, University of Liverpool, Liverpool, United Kingdom
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Adam Johnson
a Antimicrobial Pharmacodynamics and Therapeutics, University of Liverpool, Liverpool, United Kingdom
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Nicola Farrington
a Antimicrobial Pharmacodynamics and Therapeutics, University of Liverpool, Liverpool, United Kingdom
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Ruwanthi Kolamunnage-Dona
b Department of Biostatistics, Institute of Translational Medicine, University of Liverpool, Liverpool, United Kingdom
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Julie Schwartz
c Charles River Laboratories, Davis, California, USA
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Anthony Kennedy
d F2G Ltd., Eccles, United Kingdom
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Derek Law
d F2G Ltd., Eccles, United Kingdom
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Michael Birch
d F2G Ltd., Eccles, United Kingdom
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John H. Rex
d F2G Ltd., Eccles, United Kingdom
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Robert A. Bonomo
Louis Stokes Veterans Affairs Medical Center
Roles: Editor
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David Andes
University of Wisconsin-Madison
Roles: Solicited external reviewer
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Ashraf Ibrahim
Harbor-UCLA Medical Center
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DOI: 10.1128/mBio.01157-17
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ABSTRACT

F901318 is an antifungal agent with a novel mechanism of action and potent activity against Aspergillus spp. An understanding of the pharmacodynamics (PD) of F901318 is required for selection of effective regimens for study in phase II and III clinical trials. Neutropenic murine and rabbit models of invasive pulmonary aspergillosis were used. The primary PD endpoint was serum galactomannan. The relationships between drug exposure and the impacts of dose fractionation on galactomannan, survival, and histopathology were determined. The results were benchmarked against a clinically relevant exposure of posaconazole. In the murine model, administration of a total daily dose of 24 mg/kg of body weight produced consistently better responses with increasingly fractionated regimens. The ratio of the minimum total plasma concentration/MIC (Cmin/MIC) was the PD index that best linked drug exposure with observed effect. An average Cmin (mg/liter) and Cmin/MIC of 0.3 and 9.1, respectively, resulted in antifungal effects equivalent to the effect of posaconazole at the upper boundary of its expected human exposures. This pattern was confirmed in a rabbit model, where Cmin and Cmin/MIC targets of 0.1 and 3.3, respectively, produced effects previously reported for expected human exposures of isavuconazole. These targets were independent of triazole susceptibility. The pattern of maximal effect evident with these drug exposure targets was also apparent when survival and histopathological clearance were used as study endpoints. F901318 exhibits time-dependent antifungal activity. The PD targets can now be used to select regimens for phase II and III clinical trials.

IMPORTANCE Invasive fungal infections are common and often lethal. There are relatively few antifungal agents licensed for clinical use. Antifungal drug toxicity and the emergence of drug resistance make the treatment of these infections very challenging. F901318 is the first in a new class of antifungal agents called the orotomides. This class has a novel mechanism of action that involves the inhibition of the fungal enzyme dihydroorotate dehydrogenase. F901318 is being developed for clinical use. A deep understanding of the relationship between dosages, drug concentrations in the body, and the antifungal effect is fundamental to the identification of the regimens to administer to patients with invasive fungal infections. This study provides the necessary information to ensure that the right dose of F901318 is used the first time. Such an approach considerably reduces the risks in drug development programs and ensures that patients with few therapeutic options can receive potentially life-saving antifungal therapy at the earliest opportunity.

FOOTNOTES

    • Received 3 July 2017
    • Accepted 11 July 2017
    • Published 22 August 2017
  • Copyright © 2017 Hope et al.

This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license .

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Pharmacodynamics of the Orotomides against Aspergillus fumigatus: New Opportunities for Treatment of Multidrug-Resistant Fungal Disease
William W. Hope, Laura McEntee, Joanne Livermore, Sarah Whalley, Adam Johnson, Nicola Farrington, Ruwanthi Kolamunnage-Dona, Julie Schwartz, Anthony Kennedy, Derek Law, Michael Birch, John H. Rex
mBio Aug 2017, 8 (4) e01157-17; DOI: 10.1128/mBio.01157-17

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Pharmacodynamics of the Orotomides against Aspergillus fumigatus: New Opportunities for Treatment of Multidrug-Resistant Fungal Disease
William W. Hope, Laura McEntee, Joanne Livermore, Sarah Whalley, Adam Johnson, Nicola Farrington, Ruwanthi Kolamunnage-Dona, Julie Schwartz, Anthony Kennedy, Derek Law, Michael Birch, John H. Rex
mBio Aug 2017, 8 (4) e01157-17; DOI: 10.1128/mBio.01157-17
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KEYWORDS

Acetamides
antifungal agents
Aspergillus fumigatus
Drug Resistance, Multiple, Fungal
Invasive Pulmonary Aspergillosis
Piperazines
Pyrimidines
Pyrroles
Aspergillus fumigatus
antifungal agents
antifungal resistance
antifungal susceptibility testing
drug discovery
laboratory animals
pharmacodynamics
pharmacokinetics
pharmacology
pneumonia
pulmonary infection

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