Human Transbodies to HCV NS3/4A Protease Inhibit Viral Replication and Restore Host Innate Immunity
Autor: | Kanyarat Thueng-in, Potjanee Srimanote, Surasak Jittavisutthikul, Wanpen Chaicumpa, Rolf G. Werner, Jeeraphong Thanongsaksrikul, Watee Seesuay |
---|---|
Jazyk: | angličtina |
Rok vydání: | 2016 |
Předmět: |
0301 basic medicine
lcsh:Immunologic diseases. Allergy hepatitis C virus Phage display medicine.medical_treatment viruses Immunology NS3/4A protease Biology Virus 03 medical and health sciences Single chain antibody (ScFv) medicine Immunology and Allergy single chain antibody innate immunity Original Research NS3 Innate immune system Protease cell-penetrating antibody (transbody) virus diseases qRT-PCR Virology digestive system diseases NS2-3 protease qPCR 030104 developmental biology Viral replication biology.protein Antibody phage display lcsh:RC581-607 hepatitis C virus (HCV) |
Zdroj: | Frontiers in Immunology, Vol 7 (2016) Frontiers in Immunology |
ISSN: | 1664-3224 |
DOI: | 10.3389/fimmu.2016.00318 |
Popis: | A safe and effective direct acting anti-hepatitis C virus (HCV) agent is still needed. In this study, human single chain variable fragments of antibody (scFvs) that bound to HCV NS3/4A protein were produced by phage display technology. The engineered scFvs were linked to nonaarginines (R9) for making them cell penetrable. HCV-RNA-transfected Huh7 cells treated with the transbodies produced from four different transformed E. coli clones had reduced HCV-RNA inside the cells and in the cell spent media, as well as fewer HCV foci in the cell monolayer compared to the transfected cells in culture medium alone. The transbodies-treated transfected cells also had up-expression of the genes coding for the host innate immune response, including TRIF, TRAF3, IRF3, IL-28B, and IFN-β. Computerized homology modeling and intermolecular docking predicted that the effective transbodies interacted with several critical residues of the NS3/4A protease, including those that form catalytic triads, oxyanion loop, and S1 and S6 pockets, as well as a zinc-binding site. Although insight into molecular mechanisms of the transbodies need further laboratory investigation, it can be deduced from the current data that the transbodies blocked the HCV NS3/4A protease activities, leading to the HCV replication inhibition and restoration of the virally suppressed host innate immunity. The engineered antibodies should be tested further for treatment of HCV infection either alone, in combination with current therapeutics, or in a mixture with their cognates specific to other HCV proteins. |
Databáze: | OpenAIRE |
Externí odkaz: |