Metabolism by Aldehyde Oxidase: Drug Design and Complementary Approaches to Challenges in Drug Discovery

Manevski, Nenad; King, Leslie A.; Pitt, William R.; Lecomte, Fabien; Toselli, Francesca

doi:10.1021/acs.jmedchem.9b00875

Cited by 79 publications

(77 citation statements)

References 236 publications

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“…25 Potential DDIs between these drugs and favipiravir should be carefully monitored. Several drugs, such as citalopram, 26 zaleplon, 27 famciclovir, 28 and sulindac, 29 are also metabolized by AO. In vitro study shows that favipiravir is a mechanism based inhibitor of AO in a concentration-dependent manner between 3.14 and 942 µg/mL 15 and the previous clinical study showed a mean steady-state trough concentration of 46.1 µg/ mL in the treatment of EVD.…”

Section: Regarding Potential Drug-drug Interaction In Pharmacokineticsmentioning

confidence: 99%

Favipiravir: Pharmacokinetics and Concerns About Clinical Trials for 2019‐nCoV Infection

Chen

2020

Clin Pharma and Therapeutics

352

292

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such as interferon-ɑ, lopinavir/ ritonavir, ribavirin, and chloroquine phosphate, some clinical trials focusing on virus RNA-dependent RNA polymerase (RdRp) inhibitors have been registered and initiated. Favipiravir, a purine nucleic acid analog and potent RdRp inhibitor approved for use in influenza, is also considered in several clinical trials. Herein, we summarized the pharmacokinetic characteristics of favipiravir and possible drug-drug interactions from the view of drug metabolism. We hope this will be helpful for the design of clinical trials for favipiravir in COVID-2019, as data regarding in vitro virus inhibition and efficacy in preclinical animal studies are still not available.[Correction added on 30 April 2020, after first online publication: The first sentence in Abstract has been changed to 'An outbreak of 2019-nCoV infection has spread across the world'].

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Section: Regarding Potential Drug-drug Interaction In Pharmacokineticsmentioning

confidence: 99%

Favipiravir: Pharmacokinetics and Concerns About Clinical Trials for 2019‐nCoV Infection

Chen

2020

Clin Pharma and Therapeutics

352

292

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“…9,22 Many AO substrates report poor PKs with rapid metabolism and failed drug development. [23][24][25] Therefore, the auto-inhibition of AO is speculated to be necessary to maintain significant FPV concentration.…”

Section: Pharmacokinetics Of Fpv In Severe Covid-19mentioning

confidence: 99%

Pharmacokinetics of Favipiravir in Critically Ill Patients With COVID‐19

Irie

Nakagawa

Fujita

et al. 2020

Clinical Translational Sci

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Since December 2019, a novel coronavirus (severe acute respiratory syndrome‐coronavirus 2 (SARS‐CoV‐2)) infection has been rapidly spreading worldwide and causing the respiratory illness, coronavirus disease 2019 (COVID‐19). The antiretroviral drug favipiravir (FPV) has been experimentally used for COVID‐19 treatment since March 2020 in Japan. However, the pharmacokinetics of FPV in critically ill patients is unknown. We measured the serum concentration of FPV using high‐performance liquid chromatography in patients with severe COVID‐19 who were admitted to the intensive care unit and placed on mechanical ventilation. The patients were administered 1,600 mg of FPV twice daily on day 1, followed by 600 mg twice daily from day 2 to day 5 (or more if needed). Suspensions of FPV tablets were administered through a nasogastric tube. Seven patients were enrolled in this study. Forty‐nine blood samples were obtained from the eligible patients to evaluate FPV concentration. The FPV trough (after 8–12 hours) concentrations of most samples were lower than the lower limit of quantification (1 µg/mL) and half‐maximal effective concentration (9.7 µg/mL) against SARS‐CoV‐2 previously tested in vitro. FPV trough concentration in critically ill patients was much lower than that of healthy subjects in a previous clinical trial, which is a cause for great concern. Further study is required to determine the optimal strategy for treatment of patients with severe COVID‐19.

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“…Some compounds generate genotoxicity without metabolic activation, whereas other compounds need metabolic activation to produce their genotoxic effect, such as N-nitrosodimethylamine [92]. When a compound undergoes metabolic activation, it changes the structure or electric charge of the original chemical [93,94]; given this fact, metabolites are usually more hydrophilic than the parental compounds. These metabolites are more likely to bind to DNA, leading to corrupt replication.…”

Section: Genotoxicitymentioning

confidence: 99%

Application of In Vitro Metabolism Activation in High-Throughput Screening

Ooka

Lynch

Xia

2020

IJMS

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In vitro methods which incorporate metabolic capability into the assays allow us to assess the activity of metabolites from their parent compounds. These methods can be applied into high-throughput screening (HTS) platforms, thereby increasing the speed to identify compounds that become active via the metabolism process. HTS was originally used in the pharmaceutical industry and now is also used in academic settings to evaluate biological activity and/or toxicity of chemicals. Although most chemicals are metabolized in our body, many HTS assays lack the capability to determine compound activity via metabolism. To overcome this problem, several in vitro metabolic methods have been applied to an HTS format. In this review, we describe in vitro metabolism methods and their application in HTS assays, as well as discuss the future perspectives of HTS with metabolic activity. Each in vitro metabolism method has advantages and disadvantages. For instance, the S9 mix has a full set of liver metabolic enzymes, but it displays high cytotoxicity in cell-based assays. In vitro metabolism requires liver fractions or the use of other metabolically capable systems, including primary hepatocytes or recombinant enzymes. Several newly developed in vitro metabolic methods, including HepaRG cells, three-dimensional (3D) cell models, and organ-on-a-chip technology, will also be discussed. These newly developed in vitro metabolism approaches offer significant progress in dissecting biological processes, developing drugs, and making toxicology studies quicker and more efficient.

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Metabolism by Aldehyde Oxidase: Drug Design and Complementary Approaches to Challenges in Drug Discovery

Cited by 79 publications

References 236 publications

Favipiravir: Pharmacokinetics and Concerns About Clinical Trials for 2019‐nCoV Infection

Favipiravir: Pharmacokinetics and Concerns About Clinical Trials for 2019‐nCoV Infection

Pharmacokinetics of Favipiravir in Critically Ill Patients With COVID‐19

Application of In Vitro Metabolism Activation in High-Throughput Screening

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