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Printable Handouts
Navigable Slide Index
- Introduction
- The hepatitis C virus
- The HCV genome
- The HCV replication cycle
- Current standard therapy
- Interferon development
- Therapeutic failure of current standard therapy
- Ribavirin
- Ribavirin mechanism of action
- Antiviral and GTP depletion correlation
- Differential response to standard therapy
- Selective inhibitors of HCV replication
- The NS2 cysteine protease
- The HCV NS3 serine protease
- NS3 protease product based inhibitors
- Proof of concept with BILN-2061 (Ciluprevir)
- Telaprevir monotherapy
- Telaprevir + PEG-IFN + RBV
- Other protease inhibitors of HCV in development
- Protease inhibitors resistance mutations
- Protease inhibitor - TMC435350
- The NS3 helicase as an antiviral target
- NS4A/NS3 inhibitors
- NS4B as an antiviral target
- NS5A as an antiviral target
- NS5A inhibitor (BMS-790052)
- The NS5B RNA dependent RNA polymerase
- Nucleoside inhibitors
- Non-nucleoside HCV inhibitors (1)
- Non-nucleoside HCV inhibitors (2)
- Non-nucleoside HCV inhibitors (3)
- Non-nucleoside HCV inhibitors (4)
- Non-nucleoside NS5B combination therapy
- Imidazopyridines (Tegobuvir)
- Tegobuvir + Telaprevir
- Triple combinations
- Cyclophilin binding HCV inhibitor
- Alisporivir efficiently clears HCV replicon
- Alisporivir combination with Telaprevir
- Selecting Alisporivir resistant replicons
- Alisporivir resistance with other HCV inhibitors
- D320E contributes most to the resistance
- Prevalence of D320E in euHCV database
- Role of NS5A or NS5B in resistance
- Swapping of NS5A results in resistance transfer
- Wild type and CypA knock down studies
- Impact of mutations in Alisporivir resistant NS5A
- Cis-trans isomerase activity of cyclophilins
- D320E peptide mutation effect on cis-trans
- Working hypothesis
- Conclusion
Topics Covered
- The HCV genome and replication cycle
- Interferon development
- Ribavirin
- Antiviral and GTP depletion correlation
- Selective inhibitors of HCV replication
- The NS2 cysteine and the NS3 serine proteases
- Protease inhibitors
- The NS3 helicase as an antiviral target
- NS4A/NS3, NS4B and NS5A as antiviral targets
- The NS5B RNA dependent RNA polymerase
- Nucleoside and non-nucleoside HCV inhibitors
- Double and triple combination therapies
- Debio-025
- Resistance to HCV inhibitors
- D320E peptide mutation effect
- Role of NS5A or NS5B in resistance
- Wild type and CypA knock down studies
- Cis-trans isomerase activity of cyclophilins
Links
Series:
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Therapeutic Areas:
Talk Citation
Neyts, J. (2011, August 31). Towards the development of potent therapy against the hepatitis C virus [Video file]. In The Biomedical & Life Sciences Collection, Henry Stewart Talks. Retrieved December 27, 2024, from https://doi.org/10.69645/XPHQ1534.Export Citation (RIS)
Publication History
Financial Disclosures
- Prof. Johan Neyts has not informed HSTalks of any commercial/financial relationship that it is appropriate to disclose.
Towards the development of potent therapy against the hepatitis C virus
A selection of talks on Infectious Diseases
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