2007
DOI: 10.1111/j.1365-2125.2007.02984.x
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Exposure–response analysis reveals that clinically important toxicity difference can exist between bioequivalent carbamazepine tablets

Abstract: WHAT IS ALREADY KNOWN ABOUT THIS SUBJECT• The occurrence of central nervous system-related adverse effects has been apparently related to the absorption rate of carbamazepine (CBZ).• However, the differing absorption rate metrics of four carbamazepine formulations in a bioequivalence study were unclearly associated with the incidence of adverse effects. WHAT THIS STUDY ADDS• The relationship between the incidence of most neurological adverse effects and the absorption rate of CBZ was quantitatively established… Show more

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Cited by 33 publications
(16 citation statements)
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“…Many such modified-release products employ a multiphasic design that combines both immediate-and extended-release formulation components to achieve a quick onset of action followed by a sustained response (22). The early exposure measure such as partial area has been shown to serve as an excellent tool to characterize the PK and PD relationship (or correlation) during drug development (23). It is to be noted that the use of partial AUC as an early exposure can be truncated at reference T max or at an early time other than T max .…”
Section: Use Of Pauc As Early Exposure Measurementioning
confidence: 99%
“…Many such modified-release products employ a multiphasic design that combines both immediate-and extended-release formulation components to achieve a quick onset of action followed by a sustained response (22). The early exposure measure such as partial area has been shown to serve as an excellent tool to characterize the PK and PD relationship (or correlation) during drug development (23). It is to be noted that the use of partial AUC as an early exposure can be truncated at reference T max or at an early time other than T max .…”
Section: Use Of Pauc As Early Exposure Measurementioning
confidence: 99%
“…Unfortunately, deriving a starting dose for phase I studies of anticancer drugs from preclinical animal toxicology and systemic pharmacokinetic data often proves to be the inappropriate conversion of drug doses from animal studies to human studies. The use of models to describe PK/PD data has received more and more attention from academia, industry, and regulatory authorities and is considered an advanced approach for exposure-response analysis (5) and clinical trial simulations (6). In many cases, plasma PK properties have been successfully related to pharmacological effects, thus being used as a surrogate for drug disposition at the site of action.…”
Section: Introductionmentioning
confidence: 99%
“…For example, partial AUC can be a better predictor of safety than C max when acute tolerance develops to adverse effects (22).…”
Section: Discussionmentioning
confidence: 99%