F901318 represents a novel class of antifungal drug that inhibits dihydroorotate dehydrogenase

Oliver, Jason D.; Sibley, Graham E. M.; Beckmann, Nicola; Dobb, Katharine S.; Slater, Martin J.; McEntee, Laura; Pré, Saskia du; Livermore, Joanne; Bromley, Michael; Wiederhold, Nathan P.; Hope, William; Kennedy, A. J.; Law, Derek; Birch, Mike

doi:10.1073/pnas.1608304113

Cited by 217 publications

(291 citation statements)

References 33 publications

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“…It is currently in phase II development as an intravenous and oral agent for use in systemic mould infections, with a particular emphasis on aspergillosis and scedosporiosis (NCT02856178) 8 . The mechanism of action is very well described.…”

Section: New Agents In Developmentmentioning

confidence: 99%

“…It is a potent inhibitor of Aspergillus spp. dihydroorotate dehydrogenase, which is crucially involved in fungal pyrimidine biosynthesis 8 . Humans also have this enzyme, but F901318 is a 2,000-fold more potent inhibitor of the fungal enzyme than the mammalian enzyme homologue and, with this differential inhibitory activity, its toxicity towards mammalian cells is anticipated to be very low 8 .…”

Section: New Agents In Developmentmentioning

confidence: 99%

“…dihydroorotate dehydrogenase, which is crucially involved in fungal pyrimidine biosynthesis 8 . Humans also have this enzyme, but F901318 is a 2,000-fold more potent inhibitor of the fungal enzyme than the mammalian enzyme homologue and, with this differential inhibitory activity, its toxicity towards mammalian cells is anticipated to be very low 8 . A similar phenomenon had previously been observed with an antibacterial compound, trimethoprim, which inhibits dihydrofolate reductase in both bacteria and humans with substantially different kinetics.…”

Section: New Agents In Developmentmentioning

confidence: 99%

“…A similar phenomenon had previously been observed with an antibacterial compound, trimethoprim, which inhibits dihydrofolate reductase in both bacteria and humans with substantially different kinetics. F901318 has potent anti- Aspergillus activity in treatment of animal models 8 . Although it has poor activity against yeasts in vitro , it does possess fungicidal activity against a series of moulds and most endemic (dimorphic) mycoses 8 .…”

Section: New Agents In Developmentmentioning

confidence: 99%

“…These biomarkers enable invasive mycoses to be controlled at the early stages of infection when the tissue burden of fungi is low, an important feature of effective fungal control. Third, there has been a collation of both objective and subjective opinions into a series of antifungal management guidelines 3–8 , so that health-care systems and clinicians have basic standards to help initiate and compare successful treatments and strategies. Last, the most important factor for the successful management of fungal infections is the continued development and appropriate use of both new and old antifungal drugs.…”

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confidence: 99%

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The antifungal pipeline: a reality check

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2017

Nat Rev Drug Discov

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Invasive fungal infections continue to appear in record numbers as the immunocompromised population of the world increases, owing partially to the increased number of individuals who are infected with HIV and partially to the successful treatment of serious underlying diseases. The effectiveness of current antifungal therapies — polyenes, flucytosine, azoles and echinocandins (as monotherapies or in combinations for prophylaxis, or as empiric, pre-emptive or specific therapies) — in the management of these infections has plateaued. Although these drugs are clinically useful, they have several limitations, such as off-target toxicity, and drug-resistant fungi are now emerging. New antifungals are therefore needed. In this Review, I discuss the robust and dynamic antifungal pipeline, including results from preclinical academic efforts through to pharmaceutical industry products, and describe the targets, strategies, compounds and potential outcomes.

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Section: New Agents In Developmentmentioning

confidence: 99%

Section: New Agents In Developmentmentioning

confidence: 99%

Section: New Agents In Developmentmentioning

confidence: 99%

Section: New Agents In Developmentmentioning

confidence: 99%

mentioning

confidence: 99%

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The antifungal pipeline: a reality check

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2017

Nat Rev Drug Discov

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575

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Antifungal Drugs

Seyedmousavi

2021

Burger's Medicinal Chemistry and Drug Discovery

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Invasive fungal infections are considered an expanding public health threat, worldwide. Annually, over one billion people are estimated to suffer from fungal infections and/or allergies originating from opportunistic and pathogenic fungi. Fungal diseases also kill more than 1.5 million each year. Antifungal therapy is a central component in the management of life‐threatening fungal infections. However, only few classes of FDA‐approved antifungal agents are available for therapy, which have limited efficacy, particularly in the treatment of disseminated and emerging fungal infections. These drugs include polyenes, azoles, echinocandins, and the nucleoside analogs. Depending on the strategy chosen, monotherapy and/or combination antifungal drugs can be used based on the clinical picture and the species identification of the etiologic agent. The use of antifungal drugs in the therapy of fungal diseases can lead to the development of resistance. Of note, some organisms are inherently resistant to these antifungal agents. This chapter focuses on the currently available classes of systemic antifungal drugs in clinical use, innovative strategies in reformulation and delivery of available drugs, development of new agents of known antifungal drug classes, and new drugs of synthetic antifungal drugs under preclinical and clinical investigations. We further discuss the currently available evidence for the emergence of fungal resistance against these agents.

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Antifungal Agents

Lockhart,

Berkow

2023

ClinMicroNow

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This chapter summarizes the comparative activities of the major systemic antifungal agents against important groups of fungi. It discusses the characteristics of the several other agents that can be used for the oral or parenteral treatment of superficial, subcutaneous, or systemic fungal infections. The allylamines are a group of synthetic antifungal compounds effective in the topical and oral treatment of dermatophytoses. Terbinafine is a lipophilic drug that is available for oral or topical administration. With the exception of fluconazole and isavuconazole, food has a significant effect on the absorption of azole antifungals. Itraconazole is a lipophilic triazole drug available for oral or parenteral administration. Ketoconazole is a lipophilic drug formulated for oral or topical use. The echinocandins are semisynthetic lipopeptide antifungal agents that target the fungal cell wall. Micafungin is a water‐soluble antifungal agent, derived from a fermentation product of Coleophoma empetri .

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F901318 represents a novel class of antifungal drug that inhibits dihydroorotate dehydrogenase

Cited by 217 publications

References 33 publications

The antifungal pipeline: a reality check

The antifungal pipeline: a reality check

Antifungal Drugs

Antifungal Agents

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