Literature DB >> 10486935

Extended recombinant bacterial ghost system.

W Lubitz1, A Witte, F O Eko, M Kamal, W Jechlinger, E Brand, J Marchart, W Haidinger, V Huter, D Felnerova, N Stralis-Alves, S Lechleitner, H Melzer, M P Szostak, S Resch, H Mader, B Kuen, B Mayr, P Mayrhofer, R Geretschläger, A Haslberger, A Hensel.   

Abstract

Controlled expression of cloned PhiX174 gene E in Gram-negative bacteria results in lysis of the bacteria by formation of an E-specific transmembrane tunnel structure built through the cell envelope complex. Bacterial ghosts from a variety of bacteria are used as non-living candidate vaccines. In the recombinant ghost system, foreign proteins are attached on the inside of the inner membrane as fusions with specific anchor sequences. Ghosts have a sealed periplasmic space and the export of proteins into this space vastly extends the capacity of ghosts or recombinant ghosts to function as carriers of foreign antigens. In addition, S-layer proteins forming shell-like self assembly structures can be expressed in candidate vaccine strains prior to E-mediated lysis. Such recombinant S-layer proteins carrying foreign epitopes further extend the possibilities of ghosts as carriers of foreign epitopes. As ghosts have inherent adjuvant properties, they can be used as adjuvants in combination with subunit vaccines. Subunits or other ligands can also be coupled to matrixes like dextran which are used to fill the internal lumen of ghosts. Oral, aerogenic or parenteral immunization of experimental animals with recombinant ghosts induced specific humoral and cellular immune responses against bacterial and target components including protective mucosal immunity. The most relevant advantage of recombinant bacterial ghosts as immunogens is that no inactivation procedures that denature relevant immunogenic determinants are employed in this production. This fact explains the superior quality of ghosts when compared to other inactivated vaccines. The endotoxic component of the outer membrane does not limit the use of ghosts as vaccine candidates but triggers the release of several potent immunoregulatory cytokines. As carriers, there is no limitation in the size of foreign antigens that can be inserted in the membrane and the capacity of all spaces including the membranes, peri-plasma and internal lumen of the ghosts can be fully utilized. This extended recombinant ghost system represents a new strategy for adjuvant free combination vaccines.

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Year:  1999        PMID: 10486935     DOI: 10.1016/s0168-1656(99)00144-3

Source DB:  PubMed          Journal:  J Biotechnol        ISSN: 0168-1656            Impact factor:   3.307


  12 in total

Review 1.  The Bacterial Ghost platform system: production and applications.

Authors:  Timo Langemann; Verena Juliana Koller; Abbas Muhammad; Pavol Kudela; Ulrike Beate Mayr; Werner Lubitz
Journal:  Bioeng Bugs       Date:  2010 Sep-Oct

2.  Protection of piglets by a Haemophilus parasuis ghost vaccine against homologous challenge.

Authors:  Mingming Hu; Yanhe Zhang; Fang Xie; Gang Li; Jianjun Li; Wei Si; Siguo Liu; Shouping Hu; Zhuo Zhang; Nan Shen; Chunlai Wang
Journal:  Clin Vaccine Immunol       Date:  2013-03-27

3.  Controlled bacterial lysis for electron tomography of native cell membranes.

Authors:  Xiaofeng Fu; Benjamin A Himes; Danxia Ke; William J Rice; Jiying Ning; Peijun Zhang
Journal:  Structure       Date:  2014-11-20       Impact factor: 5.006

4.  Generation of Salmonella ghost cells expressing fimbrial antigens of enterotoxigenic Escherichia coli and evaluation of their antigenicity in a murine model.

Authors:  Chan Song Kim; Jin Hur; Seong Kug Eo; Sang-Youel Park; John Hwa Lee
Journal:  Can J Vet Res       Date:  2016-01       Impact factor: 1.310

5.  Escherichia coli ghost production by expression of lysis gene E and Staphylococcal nuclease.

Authors:  W Haidinger; U B Mayr; M P Szostak; S Resch; W Lubitz
Journal:  Appl Environ Microbiol       Date:  2003-10       Impact factor: 4.792

6.  Construction of a Salmonella Gallinarum ghost as a novel inactivated vaccine candidate and its protective efficacy against fowl typhoid in chickens.

Authors:  Atul A Chaudhari; Chetan V Jawale; Sam Woong Kim; John Hwa Lee
Journal:  Vet Res       Date:  2012-05-23       Impact factor: 3.683

7.  Protective efficacy and immune responses by homologous prime-booster immunizations of a novel inactivated Salmonella Gallinarum vaccine candidate.

Authors:  Gayeon Won; Atul A Chaudhari; John Hwa Lee
Journal:  Clin Exp Vaccine Res       Date:  2016-07-29

8.  A novel method to recover inclusion body protein from recombinant E. coli fed-batch processes based on phage ΦX174-derived lysis protein E.

Authors:  Daniela Ehgartner; Patrick Sagmeister; Timo Langemann; Andrea Meitz; Werner Lubitz; Christoph Herwig
Journal:  Appl Microbiol Biotechnol       Date:  2017-04-20       Impact factor: 4.813

9.  A novel one-step expression and immobilization method for the production of biocatalytic preparations.

Authors:  Ilka Sührer; Timo Langemann; Werner Lubitz; Dirk Weuster-Botz; Kathrin Castiglione
Journal:  Microb Cell Fact       Date:  2015-11-14       Impact factor: 5.328

10.  Recombinant Salmonella Bacteria Vectoring HIV/AIDS Vaccines.

Authors:  Nyasha Chin'ombe; Vurayai Ruhanya
Journal:  Open Virol J       Date:  2013-12-30
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