【摘 要】
:
Background/aim: To establish bioequivalence of lamotrigine dispersible/chewable (CD) tablets (test) versus compressed tablets (reference).Methods: Three clinical studies were conducted in Chinese heal
【机 构】
:
Shanghai MentalHealth Center GlaxoSmithKline (Chi
【出 处】
:
第五届定量药理学与新药评价国际会议
论文部分内容阅读
Background/aim: To establish bioequivalence of lamotrigine dispersible/chewable (CD) tablets (test) versus compressed tablets (reference).Methods: Three clinical studies were conducted in Chinese healthy male subjects to investigate the bioequivalence of two different tablet formulations of lamotrigine: CD tablet versus compressed tablet.In two open-label, randomised, two-period crossover studies, which were conducted in Hong Kong (NCT01357902) and mainland China (NCT 01879423) separately, subjects received a single dose of lamotrigine CD tablet 5 mg×5 and compressed tablet 25 mg in a randomised order.There were 14 days washout period between two doses.The 3rd study, conducted in mainland China (NCT02064465), was a single dose, open-label,randomized, parallel-group study to demonstrate the bioequivalence of lamotrigine CD tablet (100mg) and compressed tablet (100mg), subject received a single dose of lamotrigine CD tablet 100mg or compressed tablet 100mg.Pharmacokinetic samples were taken for up to 9 days after each dose.Plasma was assayed for lamotrigine concentration by HPLC/MS.Pharmacokinetic data were analyzed by noncompartmental methods using WinNonlin(R) (Pharsight Corporation).Average bioequivalence criteria were applied.Results: 24 and 23 subjects completed the two crossover studies, respectively, while 137 subjects completed the parallel-group study.In all three studies, both lamotrigine DC tablets and compressed tablets were well tolerated.Bioequivalence was demonstrated between lamotrigine CD tablets and compressed tablets based on AUC(0-¥) and Cmax, as all the 90% confidence intervals of the ration of geometric means fall within the predefined equivalence limits of.Conclusions: Three studies conducted in Chinese healthy male subjects demonstrated that lamotrigine CD tablets were bioequivalent to lamotrigine compressed tablets.Both formulations were well tolerated and the safety assessment did not reveal any safety concerns.Disclosure: These three bioequivalence studies were all funded by GSK.
其他文献
Objectives: The objective of this study was to estimate the population pharmacokinetics (PopPK) of voriconazole by using Nonlinear Mixed Effect Model, to identify the factors influencing the pharmacok
Neurosurgical procedures may damage the blood-brain barrier to allow morevancomycin distribution into the cerebrospinal fluid (CSF) from blood after intravenous administration.However, a large inter-s
Background: Cefoperazone/sulbactam (CPZ/SUL) is a beta-lactam and beta lactamase inhibitor combination for the treatment of respiratory tract infection.The aim of this study was to develop population
Aims: The purposes of this study were to establish population pharmacokinetic-pharmacodynamic (PopPK-PD) models of S-and R-warfarin in heart valvular replacement (HVR) patients and to provide suggesti
Therapeutic monoclonal antibodies (mAbs) represent a growing segment of the development pipeline in the pharmaceutical industry.Physiologically based pharmacokinetic (PBPK) modeling has been extensive
Background and Aim: Hepatic enzyme CYP2D6 plays an important role in metabolizing many drugs and its genetic polymorphism results in significant individual therapeutic difference.Estimating the phenot
Objective: To investigate the time-dose-response relationship of benvitimod cream after topical administration in patients with mild and moderate psoriasis vulgaris for dosage regimen exploring.Method
Ethical considerations prevent extensive clinical trials in pediatric populations;however, with the use of PBPK modeling, in vivo data from adults can be used to explore the mechanisms of drug disposi
Purpose: Histamine dihydrochloride (HDC) injection has been approved in Europe for the treatment of adults with acute myeloid leukemia (AML), used in combination therapy with the T-cell-derived cytoki
Methodological validations of metabonomic analysis are far from being perfect.This research tends to validate the possibility of Quadrupole linear ion trap (QTRAP) developing into a promising tool in