%0 PDF %T Evaluation of the potential inhibition effect of Paritaprevir on UGT 1A1 enzyme activity using human liver microsomes %A Alam, Novera. %D 2017-09-05T11:33:02.844-04:00 %8 2017-09-05 %R http://localhost/files/m039kh17c %X Abstract: Abstract The treatment landscape of chronic hepatitis C (HCV) has changed substantially over the last decade with the introduction of direct-acting antiviral drugs, creating more options to treat the disease. However, the importance of clinically relevant drug-drug interaction remains a challenge. Paritaprevir has been a successful candidate when used in a multidrug regimen for the treatment of HCV. However, its metabolic pathway overlaps with that of many other drugs, resulting in increased exposure of the substrate to the enzymes. A previous clinical study has shown that oral contraceptives containing 0.035mg of ethinyl estradiol (EE) when given with Viekirex (Ombitasvir/paritaprevir/ritonavir) increased the ethinyl estradiol Cmax by 16%, AUC 6% and Cmin 12%, which is a small change. Paritaprevir Cmax, AUC, and Cmin decreased by 30%, 34%, and 13% respectively. This can result in treatment failure or in some cases a health risk issue. Co-administration of EE with Viekirex is contraindicated due to increase ALT level in blood. The objective of this study was to evaluate the inhibitory effect of paritaprevir on UGT 1A1 isoforms to identify the mechanism of inhibition of ethinyl estradiol metabolism. We also wanted to relate the findings to different pharmacokinetic models to evaluate whether the interaction was clinically significant. An in vitro study was done in human liver microsomes to evaluate biotransformation of EE into its glucuronide metabolites (EE-3-O-G, EE-17-O-G). The inhibition of metabolite formation rates by paritaprevir was evaluated using different kinetic models. EE-3-O-G, the major metabolite, demonstrated substrate inhibition characteristics. Paritaprevir inhibited EE with an IC50 of 14.5±1.02 µM. Probenecid was used as a positive control inhibitor with, an IC50 1.4±1.6 mM. The time-dependent inhibition study, in which the inhibitor was pre-and not pre-exposed to the enzyme prior to substrate addition, showed a very similar inhibitory concentration. The inhibition constant (ki) value for paritaprevir on average was 20.6µM (≥ IC50). The pattern of inhibition indicated that the inhibition was reversible with competitive characteristics. The ratio of in vivo maximum concentration of paritaprevir to in vitro ([I]/ki) was 0.01658, indicating that a clinically significant drug-drug interaction is unlikely.; Thesis (M.S.)--Tufts University, 2017.; Submitted to the Dept. of Pharmacology and Drug Development.; Advisors: David Greenblatt, and Margery Beinfeld.; Keyword: Pharmacology. %[ 2022-10-12 %9 Text %~ Tufts Digital Library %W Institution