PK Analysis in Toxicokinetic Studies

What is the most appropriate way to naively pool plasma concentrations for noncompartmental pharmacokinetic analysis of data obtained in routine toxicokinetic studies in rodents? Typically, many individual plasma concentrations are below the limit of quantification (BQL) at this stage of drug development. A typical study design is as follows: 6 rats per sex per dose are divided into two sets of 3. A maximum of 3 blood samples is obtained from each set on an alternating basis. Blood sampling times are 0.5, 1, 2, 4, 6 and 8 hr after dosing. Is it appropriate to substitute missing BQL values with zero, obtain the mean, then determine the pharmacokinetic parameters? Is there a superior method for summarizing the data? Should NONMEM be used? I look forward to your comments. Sincerely, Derek A. Ganes, Ph.D.

> What is the most appropriate way to naively pool plasma > concentrations for noncompartmental pharmacokinetic analysis > of data obtained in routine toxicokinetic studies in > rodents? There is no *appropriate way* to naively pool etc.! But less naive methods may be useful. > Is it appropriate to substitute missing BQL values with > zero, obtain the mean, then determine the pharmacokinetic > parameters? NO. (some questions are very easy to answer) Reason - Not so quick to write. BQL means less than some non-zero value. If you think your errors inmeasurement may be proportional to conc then putting a zero in is a long way from non-zero. > Is there a superior method for summarizing the > data? Should NONMEM be used? I look forward to your > comments. NONMEM could be used. If I understand your design each rat may have more than one conc measured. Thats all you need to get started on a non-naive analysis. Nick Holford