1.Optimizing the dosing regimen of aripiprazole microspheres by popu-lation pharmacokinetic modeling and simulation
Qingheng MENG ; Zhihui HAN ; Qi LEI ; Bin CHEN ; Xia YIN ; Haitang HU ; Hongxia LIU ; Qingshan ZHENG ; Ling XU ; Qin HUANG
Chinese Journal of Clinical Pharmacology and Therapeutics 2025;30(4):493-500
AIM:To optimize the clinical dosage and administration regimen of a novel long-acting injectable aripiprazole microsphere(LZMT05)using plasma concentration data from two clinical trials.METHODS:Plasma concentrations were collected from 196 schizophrenia patients administered LZMT05,and a population pharmacokinetic(Pop-PK)model was developed.The therapeutic window was defined as the steady-state trough-to-peak concentration range(94.0-534 ng/mL)of oral ar-ipiprazole.Multiple clinical scenarios were simulat-ed to identify the optimal regimen.RESULTS:A one-compartment model with dual first-order ab-sorption and first-order elimination characterized LZMT05 pharmacokinetics.Covariates like sex and CYP2D6 genotype were integrated into the final model.Simulations demonstrated that switching from 10 mg oral aripiprazole to 350 mg LZMT05 ev-ery 4 weeks sustained concentrations within the therapeutic window with minimal peak-to-trough fluctuations.CONCLUSION:The PopPK-guided opti-mized LZMT05 regimen maintained drug exposure within the therapeutic window,suggesting favor-able efficacy and safety.
2.Optimizing the dosing regimen of aripiprazole microspheres by popu-lation pharmacokinetic modeling and simulation
Qingheng MENG ; Zhihui HAN ; Qi LEI ; Bin CHEN ; Xia YIN ; Haitang HU ; Hongxia LIU ; Qingshan ZHENG ; Ling XU ; Qin HUANG
Chinese Journal of Clinical Pharmacology and Therapeutics 2025;30(4):493-500
AIM:To optimize the clinical dosage and administration regimen of a novel long-acting injectable aripiprazole microsphere(LZMT05)using plasma concentration data from two clinical trials.METHODS:Plasma concentrations were collected from 196 schizophrenia patients administered LZMT05,and a population pharmacokinetic(Pop-PK)model was developed.The therapeutic window was defined as the steady-state trough-to-peak concentration range(94.0-534 ng/mL)of oral ar-ipiprazole.Multiple clinical scenarios were simulat-ed to identify the optimal regimen.RESULTS:A one-compartment model with dual first-order ab-sorption and first-order elimination characterized LZMT05 pharmacokinetics.Covariates like sex and CYP2D6 genotype were integrated into the final model.Simulations demonstrated that switching from 10 mg oral aripiprazole to 350 mg LZMT05 ev-ery 4 weeks sustained concentrations within the therapeutic window with minimal peak-to-trough fluctuations.CONCLUSION:The PopPK-guided opti-mized LZMT05 regimen maintained drug exposure within the therapeutic window,suggesting favor-able efficacy and safety.
3.Quality control of clinical data management based on EDC.
Hongxia LIU ; Yinghua LV ; Maosheng ZHOU ; Qingheng MENG ; Junchao CHEN ; Yingchun HE ; Qingshan ZHENG
Acta Pharmaceutica Sinica 2015;50(11):1470-3
With the wide application of electronic data management (EDC), the data management is shifting to a new mode. In order to recognize the advantages of EDC, we choose 20 representative registered clinical trials, which involve 5 404 subjects and 321 sites. We found that EDC has many beneficial impacts on the course of clinical trial data management, including the process of data collection, data cleaning, data quality control and clinical trial decision-making. The result also provides a reference for the adoption of EDC in clinical trials.
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