2012
DOI: 10.1002/bdd.1771
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Utility of a physiologically–based pharmacokinetic (PBPK) modeling approach to quantitatively predict a complex drug–drug–disease interaction scenario for rivaroxaban during the drug review process: implications for clinical practice

Abstract: Background: Rivaroxaban is an oral Factor Xa inhibitor. The primary objective of this communication was to quantitatively predict changes in rivaroxaban exposure when individuals with varying degrees of renal impairment are co-administered with another drug that is both a P-gp and a moderate CYP3A4 inhibitor. Methods: A physiologically based pharmacokinetic (PBPK) model was developed to simulate rivaroxaban pharmacokinetics in young (20-45 years) or older (55-65 years) subjects with normal renal function, mild… Show more

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Cited by 88 publications
(107 citation statements)
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References 35 publications
(41 reference statements)
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“…AKI would cause a sudden decrease in kidney function and hence the rapid accumulation of the NOACs, particularly for those for which the kidneys are the major route of excretion, such as dabigatran. 36,37 Our findings need to be interpreted within the limitations of the study design. We pooled the results of a group of studies that were not intended to explore bleeding outcomes in a subgroup of patients with CKD.…”
Section: Discussionmentioning
confidence: 89%
“…AKI would cause a sudden decrease in kidney function and hence the rapid accumulation of the NOACs, particularly for those for which the kidneys are the major route of excretion, such as dabigatran. 36,37 Our findings need to be interpreted within the limitations of the study design. We pooled the results of a group of studies that were not intended to explore bleeding outcomes in a subgroup of patients with CKD.…”
Section: Discussionmentioning
confidence: 89%
“…With the advancement of science and shrinking budgets for performing expensive clinical studies, more and more pharmaceutical companies are relying on modeling and simulation before embarking upon any clinical study. There has been an increasing support and encouragement from regulatory authorities on this front as well [25][26][27]. Modeling and simulation can be a very promising and effective approach, however, one should recognize the fact that without proper mechanistic insight into any model considerations, it can act as a double-edged sword.…”
Section: Simcypmentioning
confidence: 99%
“…In this context, between July 2008 and June 2010, the Office of Clinical Pharmacology at CDER, FDA, reviewed several IND and NDA submissions that incorporated PBPK simulations (18). Examples where PBPK approaches have been used to simulate PK in different populations and/or to justify dose adjustments/selection, include simulation of paediatric PK (78-82) and patient PK (83-85) from healthy volunteer data and prediction of the effects of organ impairment on PK (75)(76)(77)86,87).…”
Section: Application Of Pbpk Methodologies For Pk and Dose Predictionmentioning
confidence: 99%
“…In later drug development stages, the model can be updated with animal data specific to the therapeutic mAb to enable translation from preclinical species to human populations. We will illustrate fit- Prospective prediction of first-in-human PK in healthy volunteers (72)(73)(74) Retrospective prediction of first-in-human PK in healthy volunteers (8-11, 16,71) Prediction of PK in paediatric populations (78)(79)(80)(81)(82) Prediction of PK in patients with hepatic impairment/ liver cirrhosis (75,76) Prediction of PK in patients with renal impairment (77,86,87) Predictions of PK in other patient populations (83)(84)(85) Predictions of PK in polymorphic populations (88) for-purpose PBPK models using one example from literature and one in-house example. Adalimumab is an anti-TNF-alpha mAb approved for the treatment of rheumatoid arthritis (RA), an autoimmune disease which leads to inflammation of joints.…”
Section: Large Molecule Pbpk Modelsmentioning
confidence: 99%