Compare exposure parameters of three amantadine (AMT) formulations using an integrated population pharmacokinetic (PK) model.

Currently, three distinct AMT products are available in the US to treat manifestations of Parkinson’s disease [PD]: the original immediate-release (IR) formulation (AMT-IR, [Symmetrel] administered 2-3 times daily), and two extended-release (ER) formulations; one with an IR component (AMT-IR/ER [Osmolex ER], administered once/day morning) and one with delayed-release technology (AMT-DR/ER [Gocovri], administered once/day bedtime)). While differences in drug-release mechanisms and indications render the products non-interchangeable, little comparative PK data exist.

Data from three phase 1 (PK healthy control) and one phase 2 (PD patient) studies (including 5906 PK measurements from 125 subjects) were used to develop a population PK model. Covariates included age, BMI, weight, and creatinine clearance. The model was then used to generate predicted steady state AMT concentration-time profiles at recommended product maintenance dosages.

Drug absorption was formulation specific. Drug disposition was adequately described by a one‑compartment model with first-order elimination. Creatinine clearance and body mass were shown to impact amantadine PK. Median model-predicted, steady-state Cmax (ng/mL) for the maintenance dosages: AMT-IR 81mg BID, AMT-IR 81 mg TID, AMT-IR/ER 193mg, AMT-IR/ER 258mg and AMT‑DR/ER 274mg, were: 667, 979, 770, 1014, and 1109, respectively; median model-predicted, steady-state AUC_0‑24 (ng/mL*hr) were: 12494, 18262, 14191, 18439, and 21575, respectively. Concentrations were higher over the first half of the waking day for AMT‑DR/ER vs. AMT-IR and were more similar for AMT-IR/ER vs. AMT-IR.