Influence Of Abcb11 And Hnf4 Alpha Genes On Daclatasvir Plasma Concentration: Preliminary Pharmacogenetic Data From The Kineti-C Study

Background: Daclatasvir is an inhibitor of HCV non-structural 5A protein and is a P-glycoprotein substrate. Pharmacogenetics has had a great impact on previous anti-HCV therapies, particularly considering the association of IL-28B polymorphisms with dual therapy outcome.Objectives: We investigated the association between daclatasvir plasma concentrations at 2 weeks and 1month of therapy and genetic variants (SNPs) in genes encoding transporters and nuclear factors (ABCB1, ABCB11 and HNF4 alpha).Patients and methods: Allelic discrimination was achieved through real-time PCR, whereas plasma concentrations were evaluated through LC-MS/MS.Results: Fifty-two patients were analysed, all enrolled in the Kineti-C study. HNF4 alpha 975 C>G polymorphism was found to be associated with the daclatasvir plasma concentrations at 2 weeks (P=0.009) and 1month of therapy (P=0.006). Linear regression analysis suggested that, at 2 weeks of therapy, age, baseline BMI and haematocrit were significant predictors of daclatasvir concentrations, whereas at 1month of therapy ABCB111131 CC and HNF4 alpha CG/GG genotypes were significant predictors of daclatasvir concentrations.Conclusions: These are the first and preliminary results from our clinical study focusing on daclatasvir pharmacogenetics, showing that this approach could have a role in the era of new anti-HCV therapies.