An extension of biorelevant fed-state dissolution tests to clinical pharmacokinetics - A study on gastrointestinal factors influencing rivaroxaban exposure and efficacy in atrial fibrillation patients

被引:4
|
作者
Romanski, Michal [1 ]
Giebultowicz, Joanna [2 ,7 ]
Gniazdowska, Elzbieta [2 ,6 ]
Piotrowski, Roman [3 ]
Zuk, Anna [3 ]
Kulakowski, Piotr [3 ]
Paszkowska, Jadwiga [4 ]
Myslitska, Daria [4 ]
Sczodrok, Jaroslaw [5 ]
Garbacz, Grzegorz [4 ,5 ]
Danielak, Dorota [1 ]
机构
[1] Poznan Univ Med Sci, Dept Phys Pharm & Pharmacokinet, 3 Rokietnicka St, PL-60806 Poznan, Poland
[2] Med Univ Warsaw, Dept Drugs Chem Pharmaceut & Biomed Anal, 1 Banacha St, PL-02097 Warsaw, Poland
[3] Grochowski Hosp, Postgrad Med Sch, Dept Cardiol, 51-59 Grenadierow St, PL-04073 Warsaw, Poland
[4] Physiolut Polska, 74 Piłsudskiego St, PL-50020 Wroclaw, Poland
[5] Physiolution GmbH, 49a Walther Rathenau Str, D-17489 Greifswald, Germany
[6] Lukasiewicz Res Network, Ind Chem Inst, 8 Rydygiera, PL-01793 Warsaw, Poland
[7] Med Univ Warsaw, Dept Drugs Chem, 1 Banacha St, PL-02097 Warsaw, Poland
关键词
Atrial fibrillation biopredictive dissolution; Fed state; In-vitro-in-vivo modeling; Pharmacotherapy efficiency; Population pharmacokinetics; IN-VITRO; ABSORPTION; MODEL; WATER; DRUGS; RECOMMENDATIONS; PERFORMANCE; SIMULATION; INHIBITOR; WARFARIN;
D O I
10.1016/j.ijpharm.2023.123626
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
A direct oral anticoagulant rivaroxaban fails to prevent stroke and systemic embolism in one-to-several percent of patients with nonvalvular atrial fibrillation (NVAF), but the reasons are unknown. The study used semimechanistic in vitro-in vivo prediction (IVIVP) modeling to explore the reasons for ineffective thrombosis prevention in NVAF patients. Steady-state drug concentrations in plasma were measured at 0 h (C-trough), 3 h (C-3h), and 12 h post-dosing in thirty-four patients treated with 20 mg rivaroxaban daily. The clinical data were compared against "virtual twins" generated with a novel IVIVP model that combined drug dissolution modeling, mechanistic description of gastric drug transit, and population pharmacokinetics defining the variability of drug disposition. The nonresponders had significantly lower C-3h and C-trough than the responders (p < 0.001) and the covariates included in the population pharmacokinetic submodel did not fully explain this difference. Simulations involving varied gastrointestinal parameters in the "virtual twins" revealed that lower small intestinal effective permeability (P-eff), rather than a slower stomach emptying rate, could explain low rivaroxaban exposure in the nonresponders. IVIVP modeling was effectively used for exploring pharmacotherapy failure. Low P-eff,P- found as a major determinant of ineffective rivaroxaban treatment, encourages further research to find (pato) physiological factors influencing suboptimal absorption.
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页数:14
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