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Anchoring interferon alpha to apolipoprotein A-I reduces hematological toxicity while enhancing immunostimulatory properties.

Hepatology. 2011; 
Fioravanti Jessica,González Iranzu,Medina-Echeverz José,Larrea Esther,Ardaiz Nuria,González-Aseguinolaza Gloria,Prieto Jesús,Berraondo P
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Recombinant Antibody Services For bioactivity assays, we used mouse rIFN alpha (CHO derived mouse, Hycult Biotechnol, Uden, Holland), isolated HDL-IA, or rIA produced by GenScript with a tag that was excised by enterokinase digestion.... Recombinant human IA was expressed and purified by GenScript. Get A Quote

摘要

Interferon alpha (IFNα) is widely used for the treatment of viral hepatitis but substantial toxicity hampers its clinical use. In this work, we aimed at improving the efficacy of IFNα therapy by increasing the IFNα half-life and providing liver tropism. We selected apolipoprotein A-I (ApoA-I) as the stabilizing and targeting moiety. We generated plasmids encoding IFNα, albumin bound to IFNα (ALF), or IFNα linked to ApoA-I (IA) and mice were treated either by hydrodynamic administration of the plasmids or by injection of the corresponding recombinant proteins or high-density lipoproteins containing IA. The plasma half-life of IA was intermediate between IFNα and ALF. IA was targeted to the liver and... More

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