Lifang Xu1, Shuang Yu2, Huining Liu2, Bowen Yi3, Guopeng Wang4, Yang Liu5. 1. Affiliated Hospital of Jiangxi University of Chinese Medicine, Jiangxi Province, Nanchang, 330006, China. 2. School of Chinese Materia Medica, Beijing University of Chinese Medicine, Beijing, 100102, China. 3. Xiyuan Hospital, China Academy of Chinese Medical Sciences, Beijing, 100091, China. yibowen0229@126.com. 4. Zhongcai Health (Beijing) Biological Technology Development Co., Ltd., Beijing, 101500, China. binglelly@163.com. 5. School of Chinese Materia Medica, Beijing University of Chinese Medicine, Beijing, 100102, China. liuyang@bucm.edu.cn.
Abstract
PURPOSE: To develop a mathematical model combined between physiologically based pharmacokinetic and BTK occupancy (PBPK-BO) to simultaneously predict pharmacokinetic (PK) and pharmacodynamic (PD) changes of acalabrutinib (ACA) and active metabolite ACP-5862 in healthy humans as well as PD in patients. Next, to use the PBPK-BO to determine the optimal dosing regimens in patients alone, with different CYP3A4 variants, when co-administration with four CYP3A4 modulators and in patients with hepatic impairment, respectively. METHODS: The PBPK-BO model was built using physicochemical and biochemical properties of ACA and ACP-5862 and then verified by observed PK and PD data from healthy humans and patients. Finally, the model was applied to determine optimal dosing regimens in various clinical situations. RESULTS: The simulations demonstrated that 100 mg ACA twice daily (BID) was the optimal dosing regimen in patients alone. Additionally, dosage regimens might be reduced to 50 mg BID in patients with five CYP3A4 variants. Moreover, the dosing regimen should be modified to 100 mg (even to 50 mg) once daily (QD) when co-administration with erythromycin or clarithromycin, and be increased to 200 mg BID with rifampicin, and but be avoided co-administration with itraconazole. Furthermore, dosage regimen simulations showed that optimal dosing might be decreased to 50 mg BID in patients with mild and moderate hepatic impairment, and be avoided taking ACA in severely hepatically impaired patients. CONCLUSION: This PBPK-BO model can predict PK and PD in healthy humans and patients and also predict the optimal dosing regimens in various clinical situations.
PURPOSE: To develop a mathematical model combined between physiologically based pharmacokinetic and BTK occupancy (PBPK-BO) to simultaneously predict pharmacokinetic (PK) and pharmacodynamic (PD) changes of acalabrutinib (ACA) and active metabolite ACP-5862 in healthy humans as well as PD in patients. Next, to use the PBPK-BO to determine the optimal dosing regimens in patients alone, with different CYP3A4 variants, when co-administration with four CYP3A4 modulators and in patients with hepatic impairment, respectively. METHODS: The PBPK-BO model was built using physicochemical and biochemical properties of ACA and ACP-5862 and then verified by observed PK and PD data from healthy humans and patients. Finally, the model was applied to determine optimal dosing regimens in various clinical situations. RESULTS: The simulations demonstrated that 100 mg ACA twice daily (BID) was the optimal dosing regimen in patients alone. Additionally, dosage regimens might be reduced to 50 mg BID in patients with five CYP3A4 variants. Moreover, the dosing regimen should be modified to 100 mg (even to 50 mg) once daily (QD) when co-administration with erythromycin or clarithromycin, and be increased to 200 mg BID with rifampicin, and but be avoided co-administration with itraconazole. Furthermore, dosage regimen simulations showed that optimal dosing might be decreased to 50 mg BID in patients with mild and moderate hepatic impairment, and be avoided taking ACA in severely hepatically impaired patients. CONCLUSION: This PBPK-BO model can predict PK and PD in healthy humans and patients and also predict the optimal dosing regimens in various clinical situations.
Authors: Terry Podoll; Paul G Pearson; Jerry Evarts; Tim Ingallinera; Elena Bibikova; Hao Sun; Mark Gohdes; Kristen Cardinal; Mitesh Sanghvi; J Greg Slatter Journal: Drug Metab Dispos Date: 2018-11-15 Impact factor: 3.922
Authors: Xia Li; Sebastian Frechen; Daniel Moj; Thorsten Lehr; Max Taubert; Chih-Hsuan Hsin; Gerd Mikus; Pertti J Neuvonen; Klaus T Olkkola; Teijo I Saari; Uwe Fuhr Journal: Clin Pharmacokinet Date: 2020-06 Impact factor: 6.447