Pharmacodynamic modeling of concentration‐effect relationships after controlled‐release carbidopa/levodopa (Sinemet CR4) in Parkinson's disease

Abstract

Eight parkinsonian patients participated in a pharmacokinetic/pharmacodynamic study of sequential doses of controlled-release carbidopa (CD)/levodopa (LD) at 4-hour intervals, with serial blood samples obtained before and after each dose. Effect measurements obtained with each blood sample included tapping and walking speed as well as a global assessment of motor function. Analysis of the data by extended least squares regression for linear, E_max, and sigmoid E_max pharmacodynamic models revealed that linear relationships do not provide the best fit between LD plasma concentrations and clinical effects after controlled-release CD/LD. The data are fit best to models that are curvilinear in nature. LD plasma concentrations greater than 2.0 μg/ml resulted in sustained effects on walking and global scores while the greatest rate of change in walking and global scores occurred at 0.9 μg/ml. LD plasma concentrations fluctuating around 0.9 μg/ml may result in the “on/off” effects seen in Parkinson's disease.