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      Bacillus subtilis as a tool for vaccine development: from antigen factories to delivery vectors

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          Abstract

          Bacillus subtilis and some of its close relatives have a long history of industrial and biotechnological applications. Search for antigen expression systems based on recombinant B. subtilis strains sounds attractive both by the extensive genetic knowledge and the lack of an outer membrane, which simplify the secretion and purification of heterologous proteins. More recently, genetically modified B. subtilis spores have been described as indestructible delivery vehicles for vaccine antigens. Nonetheless both production and delivery of antigens by B. subtilis strains face some inherent obstacles, as unstable gene expression and reduced immunogenicity that, otherwise, can be overcome by already available gene technology approaches. In the present review we present the status of B. subtilis-based vaccine research, either as protein factories or delivery vectors, and discuss some alternatives for a better use of genetically modified strains.

          Translated abstract

          Bacillus subtilis e alguns de seus parentes mais próximos possuem uma longa história de aplicações industriais e biotecnológicas. A busca de sistemas de expressão de antígenos baseados em linhagens recombinants de B. subtilis mostra-se atrativa em função do conhecimento genético disponível e ausência de uma membrana externa, o que simplifica a secreção e a purificação de proteínas heterólogas. Mais recentemente, esporos geneticamente modificados de B. subtilis foram descritos com veículos indestrutíveis para o transporte de antígenos vacinais. Todavia a produção e o transporte de antígenos por linhagens de B. subtilis encontra obstáculos, como a expressão gênica instável e imunogenicidade reduzida, que podem ser superados com o auxílio de tecnologias genéticas atualmente disponíveis. Apresentamos nesta revisão o estado atual da pesquisa em vacinas baseadas em B. subtilis, empregado tanto como fábrica de proteínas ou veículos, e discute algumas alternativas para o uso mais adequado de linhagens geneticamente modificadas.

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          Most cited references86

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          Use of T7 RNA polymerase to direct expression of cloned genes.

          F. Studier, A Rosenberg, J Dunn (1990)
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            Resistance of Bacillus Endospores to Extreme Terrestrial and Extraterrestrial Environments

            W Nicholson, N Munakata, G. Horneck (2000)
            Article 0 comments Cited 207 times – based on 0 reviews     Review now
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              Human hepatitis B vaccine from recombinant yeast

              Eugene B. Buynak, William J. McAleer, Robert Z. Maigetter (1984)
              The worldwide importance of human hepatitis B virus infection and the toll it takes in chronic liver disease, cirrhosis and hepatocarcinoma, make it imperative that a vaccine be developed for worldwide application. Human hepatitis B vaccines are presently prepared using hepatitis B surface antigen (HBsAg) that is purified from the plasma of human carriers of hepatitis B virus infection. The preparation of hepatitis B vaccine from a human source is restricted by the available supply of infected human plasma and by the need to apply stringent processes that purify the antigen and render it free of infectious hepatitis B virus and other possible living agents that might be present in the plasma. Joint efforts between our laboratories and those of Drs W. Rutter and B. Hall led to the preparation of vectors carrying the DNA sequence for HBsAg and antigen expression in the yeast Saccharomyces cerevisiae. Here we describe the development of hepatitis B vaccine of yeast cell origin. HBsAg of subtype adw was produced in recombinant yeast cell culture, and the purified antigen in alum formulation stimulated production of antibody in mice, grivet monkeys and chimpanzees. Vaccinated chimpanzees were totally protected when challenged intravenously with either homologous or heterologous subtype adr and ayw virus of human serum source. This is the first example of a vaccine produced from recombinant cells which is effective against a human viral infection.
              Article 0 comments Cited 72 times – based on 0 reviews     Review now
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                Author and article information

                Contributors
                Luís C.S. Ferreira: Role: ND
                Rita C.C. Ferreira: Role: ND
                Wolfgang Schumann: Role: ND
                Journal
                Journal ID (publisher): aabc
                Title: Anais da Academia Brasileira de Ciências
                Abbreviated Title: An. Acad. Bras. Ciênc.
                Publisher: Academia Brasileira de Ciências (Rio de Janeiro )
                ISSN: 1678-2690
                Publication date (Print): March 2005
                Volume: 77
                Issue: 1
                Pages: 113-124
                Affiliations
                [1 ] Universidade de São Paulo Brazil
                [2 ] University of Bayreuth Germany
                Article
                Publisher ID: S0001-37652005000100009
                DOI: 10.1590/S0001-37652005000100009
                SO-VID: 8cd402cd-c737-4157-b6b7-ef1d1fd13cf3
                License:

                http://creativecommons.org/licenses/by/4.0/

                History
                Product

                SciELO Brazil

                Self URI (journal page): http://www.scielo.br/scielo.php?script=sci_serial&pid=0001-3765&lng=en
                Categories
                Subject: MULTIDISCIPLINARY SCIENCES

                Keywords: vaccines,Bacillus subtilis,immunization,protein expression,vacinas,imunização,expressão de proteínas
                Data availability:
                Keywords: vaccines, Bacillus subtilis, immunization, protein expression, vacinas, imunização, expressão de proteínas

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