AI Article Synopsis

  • AST-001 is an L-isomer of serine known for its protective effects on neurological disorders, and the study aimed to develop a population pharmacokinetic model for it in healthy Koreans to help establish a dosing regimen for children.
  • The model was based on plasma concentration data from 24 healthy subjects after administering different doses of AST-001, utilizing a two-compartment model for its absorption and elimination.
  • Simulation results indicated suitable twice-daily dosing regimens for various weight groups among children, setting the stage for further testing in phase 2 trials.

Article Abstract

AST-001 is an L-isomer of serine that has protective effects on neurological disorders. This study aimed to establish a population pharmacokinetic (PK) model of AST-001 in healthy Korean to further propose a fixed-dose regimen in pediatrics. The model was constructed using 648 plasma concentrations from 24 healthy subjects, including baseline endogenous levels during 24 h and concentrations after a single dose of 10, 20, and 30 g of AST-001. For the simulation, an empirical allometric power model was applied to the apparent clearance and volume of distribution with body weight. The PK characteristics of AST-001 after oral administration were well described by a two-compartment model with zero-order absorption and linear elimination. The endogenous production of AST-001 was well explained by continuous zero-order production at a rate of 0.287 g/h. The simulation results suggested that 2 g, 4 g, 7 g, 10 g, and 14 g twice-daily regimens for the respective groups of 10-14 kg, 15-24 kg, 25-37 kg, 38-51 kg, 52-60 kg were adequate to achieve sufficient exposure to AST-001. The current population PK model well described both observed endogenous production and exogenous administration of AST-001 in healthy subjects. Using the allometric scaling approach, we suggested an optimal fixed-dose regimen with five weight ranges in pediatrics for the upcoming phase 2 trial.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9263096PMC
http://dx.doi.org/10.3389/fphar.2022.891227DOI Listing

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