Literature DB >> 17766014

A new and versatile virosomal antigen delivery system to induce cellular and humoral immune responses.

Andreas R Kammer1, Mario Amacker, Silvia Rasi, Nicole Westerfeld, Christel Gremion, Danielle Neuhaus, Rinaldo Zurbriggen.   

Abstract

The purpose of a vaccine is the induction of effective cellular and/or humoral immune responses against antigens. Because defined antigens are often poor immunogens when administered alone, an adjuvant is required to potentiate the immune response. Most of these adjuvants are designed to induce humoral immune responses, including immunopotentiating reconstituted influenza virosomes (IRIVs). IRIVs are one of the few adjuvants currently licensed for human use with the advantage of an excellent safety profile. To induce a potent cytotoxic T lymphocyte (CTL) immune response CTL epitopes have to be encapsulated into IRIVs. However, the existing encapsulation methods are inefficient or rather laborious. We have developed and characterised a new generation of influenza virosomes (TIRIVs) that induced both, strong CTL and antibody responses against specific antigens of choice. In addition, these virosomes were stabilised and offer the possibility of lyophilisation while retaining all their structural, functional and immunogenic properties after reconstitution. TIRIVs induce strong cellular and humoral immune responses and are a versatile and efficient carrier system with adjuvant properties for a variety of antigens. TIRIVs are not only stabilised but also allow easy formulation of new and/or labile T cell and B cell antigens. Considering their immunogenic properties, their flexibility and their superior storage characteristics TIRIVs provide a versatile technology platform for any vaccination strategy.

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Year:  2007        PMID: 17766014     DOI: 10.1016/j.vaccine.2007.07.052

Source DB:  PubMed          Journal:  Vaccine        ISSN: 0264-410X            Impact factor:   3.641


  13 in total

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Review 3.  Vaccine adjuvants: current challenges and future approaches.

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4.  Virosome-formulated Plasmodium falciparum AMA-1 & CSP derived peptides as malaria vaccine: randomized phase 1b trial in semi-immune adults & children.

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Journal:  PLoS One       Date:  2011-07-22       Impact factor: 3.240

5.  Chitosan nanoparticles act as an adjuvant to promote both Th1 and Th2 immune responses induced by ovalbumin in mice.

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6.  Immunogenicity of a virosomally-formulated Plasmodium falciparum GLURP-MSP3 chimeric protein-based malaria vaccine candidate in comparison to adjuvanted formulations.

Authors:  Marco Tamborrini; Sabine A Stoffel; Nicole Westerfeld; Mario Amacker; Michael Theisen; Rinaldo Zurbriggen; Gerd Pluschke
Journal:  Malar J       Date:  2011-12-13       Impact factor: 2.979

7.  Influenza T-cell epitope-loaded virosomes adjuvanted with CpG as a potential influenza vaccine.

Authors:  Peter C Soema; Sietske K Rosendahl Huber; Geert-Jan Willems; Wim Jiskoot; Gideon F A Kersten; Jean-Pierre Amorij
Journal:  Pharm Res       Date:  2014-10-25       Impact factor: 4.200

Review 8.  Plant Viruses as Nanoparticle-Based Vaccines and Adjuvants.

Authors:  Marie-Ève Lebel; Karine Chartrand; Denis Leclerc; Alain Lamarre
Journal:  Vaccines (Basel)       Date:  2015-08-05

9.  Strategies for intranasal delivery of vaccines.

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Journal:  Drug Deliv Transl Res       Date:  2012-07-12       Impact factor: 4.617

10.  Pulmonary Delivery of Virosome-Bound Antigen Enhances Antigen-Specific CD4+ T Cell Proliferation Compared to Liposome-Bound or Soluble Antigen.

Authors:  Rebecca A M Blom; Mario Amacker; R Maarten van Dijk; Christian Moser; Philip A Stumbles; Fabian Blank; Christophe von Garnier
Journal:  Front Immunol       Date:  2017-04-07       Impact factor: 7.561

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