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A protective immune response using asymmetric multi-epitope self-adjuvanting lipopeptide vaccine model
5th Asia Pacific Global Summit and Expo on Vaccines & Vaccination
July 27-29, 2015 Brisbane, Australia
Sharareh Eskandari1, Rachel J Stephenson1, David Pattinson2, Bita Sedaghat1, Saranya Chandrudu1, Simon H Apte2, Denise L Doolan2 and Istvan Toth1
Scientific Tracks Abstracts: J Vaccines Vaccin
Abstract:
Adjuvant development is crucially important area of research for improving subunit vaccines. It is important to understand the impact of physicochemical properties of vaccine on immune response to fulfil development of a delivery system with robust protection against infection and tumour. Here, we synthesised a library of lipopeptide (LP) vaccine constructs to contain an asymmetrical arrangement of peptide epitopes (OVA CD4 and OVA CD8) to determine the optimal architecture for stimulation of a potent cell mediated response. C12 or C16 lipoamino acids were included in different locations of the constructs. The constructs were self-assembled in PBS and characterised. C57BL/6 mice were immunised with vaccine constructs following adoptive transfer of congenic (CD45.1) ovalbumin specific OT-I and OT-II T cells. Frequency of proliferation of OT-I and OT-II cells in na�ve mice were determined using FACS analysis. Then, the effector function of activated OT-I cells in response to the vaccine constructs were evaluated by cytotoxic T lymphocyte assay. Following immunisation, mice were challenged by subcutaneous injection on their abdomen with tumour cells expressing ovalbumin and investigated for inhibition of tumour growth. Furthermore, an IFN-? ELISpot assay was performed to enumerate the antigen-specific effector cells secreting IFN-?. Results showed that constructs with C16 lipids at the N-terminus formed long ?-sheet fibrils and induced higher CD8+ T cell proliferation and IFN-? secretion compared with constructs containing internal placement of lipids. Constructs with small nanoparticles or beta-sheet secondary structures showed high cytolytic activity and tumour growth inhibition (Figure 1). Future direction aim to investigate the impact of these particles on humoral immune response in vivo. Figure 1. A: Asymmetric construct library showing lipid position at N-terminus or internally. B: Percentages of OVA CD8 specific lysis one week post immunisation and tumour weight 3 weeks post immunisation.
Biography :
Sharareh Eskandari is pharmacist and has completed his PhD from Isfahan University of Medical Science in pharmaceutics. She is PhD candidate in medicinal chemistry and vaccine delivery at the University of Queensland, School of Chemistry and Molecular Bioscience. She published 8 papers in reputed journals, one eBook chapter in liposomal drug delivery and had been served as responsible pharmacist in pharmaceutical industry.