Influence of switching from intravenous to oral administration on serum voriconazole concentration

Harada, Saki; Niwa, Takashi; Hoshino, Yusuke; Fujibayashi, Ayasa; Suzuki, Akio

doi:10.1111/jcpt.13352

Cited by 5 publications

(5 citation statements)

References 30 publications

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“…to p.o. route of administration has the potential to lower the plasma exposure to ineffectual levels and result in treatment failure ( 31 , 32 ). However, the i.v.…”

Section: Discussionmentioning

confidence: 99%

Safety and Pharmacokinetics of Intravenous and Oral Fosmanogepix, a First-in-Class Antifungal Agent, in Healthy Volunteers

Hodges

Ople

Wedel

et al. 2023

Antimicrob Agents Chemother

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Fosmanogepix (FMGX, APX001), a first-in-class, intravenous (i.v.) and oral (p.o.) antifungal prodrug candidate is currently in clinical development for the treatment of invasive fungal infections. Manogepix (MGX, APX001A), the active moiety of FMGX, interferes with cell wall synthesis by targeting fungal glycosylphosphatidylinositol-anchored cell wall transfer protein 1, thereby causing loss of cell viability.

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“…to p.o. route of administration has the potential to lower the plasma exposure to ineffectual levels and result in treatment failure ( 31 , 32 ). However, the i.v.…”

Section: Discussionmentioning

confidence: 99%

Safety and Pharmacokinetics of Intravenous and Oral Fosmanogepix, a First-in-Class Antifungal Agent, in Healthy Volunteers

Hodges

Ople

Wedel

et al. 2023

Antimicrob Agents Chemother

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“…To confirm the optimal timing of the initial TDM, we set a stepwise cutoff for the timing of the initial TDM within a range of 3–6 days after the start of voriconazole treatment. Good to excellent bioavailability has been reported for voriconazole 21,22 . However, there are some differences in the concentrations obtained with the same dose of oral and intravenous administration.…”

Section: Methodsmentioning

confidence: 97%

“…Good to excellent bioavailability has been reported for voriconazole. 21,22 However, there are some differences in the concentrations obtained with the same dose of oral and intravenous administration. Therefore, voriconazole C min was measured following the route of administration, and the main PK analyses were conducted in patients who received oral voriconazole.…”

Section: Protocol For Tdmmentioning

confidence: 99%

Optimal timing for therapeutic drug monitoring of voriconazole to prevent adverse effects in Japanese patients

Hanai

Hamada

Oda

et al. 2023

Mycoses

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BackgroundThe optimal timing for therapeutic drug monitoring (TDM) of voriconazole in Asians, who have higher rates of poor metabolisers than non‐Asians, is unclear. This can cause unexpectedly high concentrations and delays in reaching steady‐state levels.ObjectivesTo determine the appropriate timing of TDM in Japanese patients receiving voriconazole.Patients/MethodsTrough levels (Cmin) were measured on days 3–5 (recommended timing, RT) and days 6–14 (delayed timing, DT) after starting voriconazole in patients receiving an appropriate dosage. Considering bioavailability, Cmin was only compared in patients receiving oral voriconazole.ResultsA total of 289 and 186 patients were included in the safety and pharmacokinetic analyses, respectively. There was a significant difference in Cmin measured no later than and after day 5 (3.59 ± 2.12 [RT] vs. 4.77 ± 3.88 μg/mL [DT], p = .023), whereas no significant difference was observed on cutoff day 6 (3.91 ± 2.60 vs. 4.40 ± 3.94 μg/mL, p = .465), suggesting that Cmin close to the steady‐state was achieved after day 5. DT causes a delay in achieving the therapeutic range. The hepatotoxicity rates were 21.5% and 36.8% in the RT and DT groups, respectively (p = .004); DT was an independent risk factor for hepatotoxicity.ConclusionAlthough steady‐state concentrations may not be achieved by day 5, early dose optimisation using RT can prevent hepatotoxicity in Japanese patients. TDM should be performed on days 3–5 to ensure safety. However, subsequent TDM may be necessary due to a possible further increase in Cmin.

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“…Existing treatment options may have limited use in patients with IFDs, due to poor tolerability and toxicity, suboptimal drug exposure at the site of infection, reduced bioavailability of oral formulations while switching dosage forms, 8 and pharmacokinetic interactions with other drugs. 9 In addition, switching from IV to oral formulations may lead to poor drug exposures and potentially suboptimal efficacy.…”

Section: Introductionmentioning

confidence: 99%

“…For example, switching from IV to oral voriconazole led to an 80% decrease in plasma concentrations, although both formulations were administered at the same dose. 8 In patients with ALL receiving vincristine chemotherapy, voriconazole and itraconazole coadministration resulted in significant drug–drug interactions leading to adverse drug reactions prohibiting azole use in those patients. 10 In addition, rates of resistance are increasing and MDR pathogenic fungi that are resistant to treatment with amphotericin B, azoles and echinocandins have been reported.…”

Section: Introductionmentioning

confidence: 99%

Phase 1b safety and pharmacokinetics of intravenous and oral fosmanogepix in patients with acute myeloid leukaemia and neutropenia

Cornely,

Ostermann,

Koehler

et al. 2023

Journal of Antimicrobial Chemotherapy

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Objectives Fosmanogepix (APX001), a first-in-class, intravenous (IV) and oral (PO) antifungal prodrug, is being developed to treat invasive fungal diseases (IFDs). Manogepix (APX001A; active moiety) targets fungal glycosylphosphatidylinositol-anchored cell wall transfer protein 1, inhibiting cell wall synthesis causing loss of viability. This open-label, multicentre, Phase 1b study in patients with AML and neutropenia (absolute neutrophil count <500 cells/μL; >10 days) undergoing chemotherapy aimed to assess tolerability, safety and pharmacokinetics (PK) of IV and PO fosmanogepix. Methods Of 21 adult AML patients undergoing remission induction chemotherapy, 10 received IV fosmanogepix (600 mg; q24h) and 11 received oral fosmanogepix (500 mg; q24h) over 14 days, with a 28 day follow-up. Patients also received remission induction chemotherapy [sequential high-dose cytarabine and mitoxantrone (S-HAM) or 7 + 3 regimen] for AML and IFD prophylaxis (posaconazole). A two-compartmental PK model from previous studies in healthy volunteers was fitted to manogepix plasma data. Results Of 26 fosmanogepix-related adverse events (AEs; IV: 14; PO: 12) in 9 (42.9%) patients [IV: 5 (50%); PO: 4 (36.4%)], none were serious or resulted in fosmanogepix discontinuation. Most frequently occurring fosmanogepix-related AEs were Grade 1/2 nausea [four events in three patients (14.3%)]; vomiting, ALT increase, and delirium [two events; two patients (9.5%) each]. One patient experienced fosmanogepix-related Grade 3 hypertension. Dose-corrected geometric mean ratio of AUC (PO-to-IV) was 95%. Elimination half-lives (∼2 days) were consistent with prior studies in healthy volunteers. Conclusions Fosmanogepix was safe and well tolerated in AML patients with neutropenia receiving remission induction chemotherapy. Safety and PK profiles were comparable to healthy volunteers.

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Influence of switching from intravenous to oral administration on serum voriconazole concentration

Cited by 5 publications

References 30 publications

Safety and Pharmacokinetics of Intravenous and Oral Fosmanogepix, a First-in-Class Antifungal Agent, in Healthy Volunteers

Safety and Pharmacokinetics of Intravenous and Oral Fosmanogepix, a First-in-Class Antifungal Agent, in Healthy Volunteers

Optimal timing for therapeutic drug monitoring of voriconazole to prevent adverse effects in Japanese patients

Phase 1b safety and pharmacokinetics of intravenous and oral fosmanogepix in patients with acute myeloid leukaemia and neutropenia

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