Assessing the bioequivalence of 4- and 8-mg benidipine tablets in healthy volunteers after a single oral dose

Objective: To assess the bioequivalence of a new tablet formulation of benidipine hydrochloride with reference to a marketed product.

Methods: Two groups, consisting of 24 healthy volunteers each, received a 4- or 8-mg (one or two tablets) reference benidipine hydrochloride tablet and one or two test tablets in a 2 × 2 cross-over study. There was a 6-day washout period between doses. The plasma benidipine concentration was monitored using LC/MS/MS for 8 h after the dose. The area under the plasma concentration–time curve from time 0 to the last sampling time (AUC_t) was calculated using the linear-log trapezoidal rule. The maximum plasma drug concentration (C_max) and the time to reach C_max (T_max) were compiled from the plasma concentration–time data. Analysis of variance was carried out using logarithmically transformed AUC_t and C_max, and untransformed T_max.

Results: The geometric mean AUC_t was 2·23ng/mL/h (test medication) and 2·47 ng/mL/h (reference medication) for the 4-mg tablet, and 9·57 and 9·97 ng/mL/h for the 8-mg tablet, respectively. A C_max of 1·94 and 2·01 ng/mL was achieved for the test and reference medication for the 4-mg tablet, and 5·94 and 6·53 ng/mL for the 8-mg tablet, respectively. The 90% confidence intervals for AUC_t and C_max were 0·8441–1·0481 and 0·8739–1·2037 for the 4-mg tablet, and 0·8559–1·1273 and 0·9926–1·2176 for the 8-mg tablet, respectively, satisfying the bioequivalence criteria of the US Food and Drug Administration Guidelines, and the Korea Food and Drug Administration Guidelines. These results indicate that the 4- and 8-mg tablets of benidipine are bioequivalent to the reference formulations.