Population pharmacokinetic modeling of GS‐441524, the active metabolite of remdesivir, in Japanese COVID‐19 patients with renal dysfunction

Abstract: Remdesivir, a prodrug of the nucleoside analog GS‐441524, plays a key role in the treatment of coronavirus disease 2019 (COVID‐19). However, owing to limited information on clinical trials and inexperienced clinical use, there is a lack of pharmacokinetic (PK) data in patients with COVID‐19 with special characteristics. In this study, we aimed to measure serum GS‐441524 concentrations and develop a population PK (PopPK) model. Remdesivir was administered at a 200 mg loading dose on the first day followed by 10… Show more

“…Efforts to fit more complex models to the data resulted in parameter estimates with high residual errors, which could be a result of the limited sample size in this study. Nevertheless, the developed one-compartment model showed good resemblance between the predicted and measured concentrations of remdesivir and GS-441524 and is in line with the results of Sukeishi et al for GS-441524 ( 21 ).…”

“…However, the lower elimination half-life could also be related to differences in study populations or study procedures. GS-441524 clearance in COVID-19 patients was higher than that previously reported (27.6 L/h versus 11.8 L/h), a possible result of the higher median eGFR, differences in ethnicity or the severity of disease, or the lack of remdesivir concentration data in the study population ( 21 ). The volume of distribution was larger for remdesivir and GS-441524 than that in healthy individuals, which can be explained by the high BMI of the patients in the study population or potentially disease- or treatment-related factors.…”

“…The optimal dose leading to the maximal antiviral efficacy of remdesivir in humans is currently unknown, but modeling and simulation studies suggest that the current dosing regimen might be suboptimal ( 14 , 15 ). These studies were performed using pharmacokinetic data from healthy individuals, whereas studies regarding the pharmacokinetics of remdesivir in COVID-19 patients are limited to case series with scarce sampling schedules and a single pharmacokinetic study with only GS-441524 concentrations ( 16 – 21 ).…”

Population Pharmacokinetics of Remdesivir and GS-441524 in Hospitalized COVID-19 Patients

“…Efforts to fit more complex models to the data resulted in parameter estimates with high residual errors, which could be a result of the limited sample size in this study. Nevertheless, the developed one-compartment model showed good resemblance between the predicted and measured concentrations of remdesivir and GS-441524 and is in line with the results of Sukeishi et al for GS-441524 ( 21 ).…”

“…However, the lower elimination half-life could also be related to differences in study populations or study procedures. GS-441524 clearance in COVID-19 patients was higher than that previously reported (27.6 L/h versus 11.8 L/h), a possible result of the higher median eGFR, differences in ethnicity or the severity of disease, or the lack of remdesivir concentration data in the study population ( 21 ). The volume of distribution was larger for remdesivir and GS-441524 than that in healthy individuals, which can be explained by the high BMI of the patients in the study population or potentially disease- or treatment-related factors.…”

“…The optimal dose leading to the maximal antiviral efficacy of remdesivir in humans is currently unknown, but modeling and simulation studies suggest that the current dosing regimen might be suboptimal ( 14 , 15 ). These studies were performed using pharmacokinetic data from healthy individuals, whereas studies regarding the pharmacokinetics of remdesivir in COVID-19 patients are limited to case series with scarce sampling schedules and a single pharmacokinetic study with only GS-441524 concentrations ( 16 – 21 ).…”

Population Pharmacokinetics of Remdesivir and GS-441524 in Hospitalized COVID-19 Patients

“… 26 The high volume of distribution of GS-441524 (6.36 L/kg) is consistent with this interpretation. 27 Upon comparison of differences in pharmacokinetic characteristics in plasma between humans and rats, despite different routes of drug administration, similar remdesivir and GS-441524 pharmacokinetics characteristics were observed. Remdesivir followed a rapid decline 28 and the absorption of GS-441524 appeared at the second time-point, with a slow elimination phase.…”

Biotransformation and transplacental transfer of the anti-viral remdesivir and predominant metabolite, GS-441524 in pregnant rats

“… 11 Contrary to the precautionary advice, for patients with eGFR <30 some reported studies recommend dose adjustment rather than precautionary limits. 12 On the other hand, animal studies demonstrated potential, beneficial, renal effects in reversing obstructive renal fibrosis. 13 Of note, such cohort of patients with chronic kidney disease at significant risks of acquisition and complications of COVID‐19 disease as highlighted from multiple observational studies.…”

Remdesivir for COVID‐19 pneumonia in patients with severe chronic kidney disease: A Case series and review of the literature