Drug Disposition in Subjects With Obesity: The Research Work of Darrell R. Abernethy

Abstract

In 1979, the late Dr. Darrell R. Abernethy and colleagues began a series of clinical studies aimed at understanding the pertinent determinants of drug distribution, elimination, and clearance in obesity, and how those variables are interconnected. The studies confirmed that volume of distribution (V_d ) and clearance are the principal independent biological variables, which conjointly determine elimination of half-life as a dependent variable. For drugs distributed by passive diffusion, their pharmacokinetic V_d - after correcting for plasma protein binding - was increased in obesity, depending in part on the physicochemical lipophilicity of the individual drugs, and the quantitative extent of obesity in overweight individuals. Across all studies, the ratio of mean clearance in obese divided by control groups had an overall median value of 1.21 (range, 0.75-3.11), indicating a small and variable effect of obesity on clearance, without clear directionality. Since drug clearance was not clearly related to lipophilicity or degree of obesity, the prolonged half-life of lipophilic drugs in patients with obesity was largely explained by the increased V_d . Dr. Abernethy further identified delayed attainment of steady state after initiation of multiple-dose treatment, and delayed washout after termination of dosage, as potential clinical consequences of the extended half-life in people with obesity. These consequences for specific drugs have been recently emphasized in contemporary studies of chronic dosage in subjects with obesity. Without data identifying an obesity-related change in clearance for a specific drug, maintenance doses (in milligrams) should be based on ideal weight rather than adjusted upward on the basis of total weight.

Keywords: drug accumulation; drug distribution; elimination half-life; lipophilicity; obesity; pharmacokinetics.