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Characterisation of a New Molecule Based on Two E2 Sequences from Bovine Viral Diarrhoea-mucosal Disease Virus Fused To the Human Immunoglobulin Fc Fragment.
González Pose, Alaín; Montesino Seguí, Raquel; Maura Pérez, Rafael; Hugues Salazar, Florence; Cabezas Ávila, Ignacio; Altamirano Gómez, Claudia; Sánchez Ramos, Oliberto; Roberto Toledo, Jorge.
Affiliation
  • González Pose A; Biotechnology and Biopharmaceutical Laboratory, Pathophysiology Department, School of Biological Sciences, University of Concepcion, Victor Lamas 1290, P.O. Box 160-C, 4030000 Concepcion, Chile.
  • Montesino Seguí R; Biotechnology and Biopharmaceutical Laboratory, Pathophysiology Department, School of Biological Sciences, University of Concepcion, Victor Lamas 1290, P.O. Box 160-C, 4030000 Concepcion, Chile.
  • Maura Pérez R; Biotechnology and Biopharmaceutical Laboratory, Pathophysiology Department, School of Biological Sciences, University of Concepcion, Victor Lamas 1290, P.O. Box 160-C, 4030000 Concepcion, Chile.
  • Hugues Salazar F; Biotechnology and Biopharmaceutical Laboratory, Pathophysiology Department, School of Biological Sciences, University of Concepcion, Victor Lamas 1290, P.O. Box 160-C, 4030000 Concepcion, Chile.
  • Cabezas Ávila I; Large Animal Clinic, Clinical Sciences Department, School of Veterinary Sciences, University of Concepcion, Vicente Mendez 595, P.O. Box 537, 3780000 Chillan, Chile.
  • Altamirano Gómez C; School of Biochemical Engineering, Pontifical Catholic University of Valparaiso, Valparaiso, Chile CREAS CONICYT-Regional, GORE Valparaiso, Universidad Avenue 300, Placilla, Curauma, 2340000 Valparaiso, Chile.
  • Sánchez Ramos O; Recombinant Biopharmaceuticals Laboratory, Pharmacology Department, School of Biological Sciences, University of Concepcion, Victor Lamas 1290, P.O. Box 160-C, 4030000 Concepcion, Chile.
  • Roberto Toledo J; Biotechnology and Biopharmaceutical Laboratory, Pathophysiology Department, School of Biological Sciences, University of Concepcion, Victor Lamas 1290, P.O. Box 160-C, 4030000 Concepcion, Chile.
J Vet Res ; 65(1): 27-37, 2021 Mar.
Article in En | MEDLINE | ID: mdl-33817392
INTRODUCTION: Proper conformational arrangement of the E2 molecules of bovine viral diarrhoea-mucosal disease virus (BVD-MDV) is crucial to obtain an effective recombinant vaccine candidate against the disease. In this study, we characterised a new molecule composed of two distinct sequences of the E2 glycoprotein of BVD-MDV and the Fc fragment of human immunoglobulin (BVDE2Fc). MATERIALS AND METHODS: The chimaeric protein was expressed in mammalian cell lines of different species by adenoviral transduction and purified by immobilised metal-affinity chromatography. The N-glycans were profiled by HPLC, and the BVDE2Fc immunogenicity was assessed in male mice. The antigen-antibody reactions were evaluated by ELISA. RESULTS: The MDBK cell line was selected from among five for the final production of BVDE2Fc. After purification to over 90%, the N-glycan profile showed neutral and complex oligosaccharides. The mouse immunisation induced a strong humoral response, which produced antibodies able to attach to conformational epitopes on E2 molecules, while the Fc fragment barely contributed to the immune response. Additionally, BVDE2Fc attached to antibodies from bovine sera positive to distinct BVD-MDV subtypes, whereas the loss of BVDE2Fc structure during the deglycosylation process considerably diminished those interactions. CONCLUSION: These results demonstrate that the structure of E2 molecules arranged in tandem and attached to an Fc fragment could represent a viable design for future vaccine candidates against BVD-MD.
Key words

Full text: 1 Collection: 01-internacional Database: MEDLINE Language: En Journal: J Vet Res Year: 2021 Document type: Article Affiliation country: Chile Country of publication: Poland

Full text: 1 Collection: 01-internacional Database: MEDLINE Language: En Journal: J Vet Res Year: 2021 Document type: Article Affiliation country: Chile Country of publication: Poland