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Extracellular secretion of a recombinant therapeutic peptide by Bacillus halodurans utilizing a modified flagellin type III secretion system

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dc.contributor.author Berger, E
dc.contributor.author Crampton, Michael C
dc.contributor.author Nxumalo, NP
dc.contributor.author Louw, ME
dc.date.accessioned 2012-01-20T08:34:17Z
dc.date.available 2012-01-20T08:34:17Z
dc.date.issued 2011-08
dc.identifier.citation Berger, E., Crampton, M.C., Nxumalo, N.P. et al. 2011. Extracellular secretion of a recombinant therapeutic peptide by Bacillus halodurans utilizing a modified flagellin type III secretion system. Microbial Cell Factories, Vol. 10(62), pp 1-10 en_US
dc.identifier.issn 1475-2859
dc.identifier.uri http://www.microbialcellfactories.com/content/10/1/62
dc.identifier.uri http://hdl.handle.net/10204/5519
dc.description Copyright: 2011 Berger et al; licensee BioMed Central Ltd. This is an Open Access article distributed under the terms of the Creative Commons Attribution License. Which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited. en_US
dc.description.abstract Through modification of the flagellin type III secretion pathway of Bacillus halodurans heterologous peptides could be secreted into the medium as flagellin fusion monomers. The stability of the secreted monomers was significantly enhanced through gene-targeted inactivation of host cell extracellular proteases. In evaluating the biotechnological potential of this extracellular secretion system an anti-viral therapeutic peptide, Enfuvirtide, was chosen. Currently, Enfuvirtide is synthesised utilizing 106 chemical steps. The authors used Enfuvirtide as a model system in an effort to develop a more cost-effective biological process for therapeutic peptide production. Results: An attempt was made to increase the levels of the fusion peptide by two strategies, namely strain improvement through gene-targeted knock-outs, as well as vector and cassette optimization. Both approaches proved to be successful. Through chromosomal inactivation of the spo0A, lytC and lytE genes, giving rise to strain B. halodurans BhFDL05S, the secretion of recombinant peptide fusions was increased 10-fold. Cassette optimization, incorporating an expression vector pNW33N and the N- and C-terminal regions of the flagellin monomer as an inframe peptide fusion, resulted in a further 3.5-fold increase in the secretion of recombinant peptide fusions. Conclusions: The type III flagellar secretion system of B. halodurans has been shown to successfully secrete a therapeutic peptide as a heterologous flagellin fusion. Improvements to both the strain and expression cassette led to increased levels of recombinant peptide, showing promise for a biotechnological application. en_US
dc.language.iso en en_US
dc.publisher Biomed Central en_US
dc.relation.ispartofseries Workflow request;7183
dc.subject Bacillus halodurans en_US
dc.subject Flagellin en_US
dc.subject Peptides en_US
dc.subject Enfuvirtide en_US
dc.subject Microbial cells en_US
dc.title Extracellular secretion of a recombinant therapeutic peptide by Bacillus halodurans utilizing a modified flagellin type III secretion system en_US
dc.type Article en_US
dc.identifier.apacitation Berger, E., Crampton, M. C., Nxumalo, N., & Louw, M. (2011). Extracellular secretion of a recombinant therapeutic peptide by Bacillus halodurans utilizing a modified flagellin type III secretion system. http://hdl.handle.net/10204/5519 en_ZA
dc.identifier.chicagocitation Berger, E, Michael C Crampton, NP Nxumalo, and ME Louw "Extracellular secretion of a recombinant therapeutic peptide by Bacillus halodurans utilizing a modified flagellin type III secretion system." (2011) http://hdl.handle.net/10204/5519 en_ZA
dc.identifier.vancouvercitation Berger E, Crampton MC, Nxumalo N, Louw M. Extracellular secretion of a recombinant therapeutic peptide by Bacillus halodurans utilizing a modified flagellin type III secretion system. 2011; http://hdl.handle.net/10204/5519. en_ZA
dc.identifier.ris TY - Article AU - Berger, E AU - Crampton, Michael C AU - Nxumalo, NP AU - Louw, ME AB - Through modification of the flagellin type III secretion pathway of Bacillus halodurans heterologous peptides could be secreted into the medium as flagellin fusion monomers. The stability of the secreted monomers was significantly enhanced through gene-targeted inactivation of host cell extracellular proteases. In evaluating the biotechnological potential of this extracellular secretion system an anti-viral therapeutic peptide, Enfuvirtide, was chosen. Currently, Enfuvirtide is synthesised utilizing 106 chemical steps. The authors used Enfuvirtide as a model system in an effort to develop a more cost-effective biological process for therapeutic peptide production. Results: An attempt was made to increase the levels of the fusion peptide by two strategies, namely strain improvement through gene-targeted knock-outs, as well as vector and cassette optimization. Both approaches proved to be successful. Through chromosomal inactivation of the spo0A, lytC and lytE genes, giving rise to strain B. halodurans BhFDL05S, the secretion of recombinant peptide fusions was increased 10-fold. Cassette optimization, incorporating an expression vector pNW33N and the N- and C-terminal regions of the flagellin monomer as an inframe peptide fusion, resulted in a further 3.5-fold increase in the secretion of recombinant peptide fusions. Conclusions: The type III flagellar secretion system of B. halodurans has been shown to successfully secrete a therapeutic peptide as a heterologous flagellin fusion. Improvements to both the strain and expression cassette led to increased levels of recombinant peptide, showing promise for a biotechnological application. DA - 2011-08 DB - ResearchSpace DP - CSIR KW - Bacillus halodurans KW - Flagellin KW - Peptides KW - Enfuvirtide KW - Microbial cells LK - https://researchspace.csir.co.za PY - 2011 SM - 1475-2859 T1 - Extracellular secretion of a recombinant therapeutic peptide by Bacillus halodurans utilizing a modified flagellin type III secretion system TI - Extracellular secretion of a recombinant therapeutic peptide by Bacillus halodurans utilizing a modified flagellin type III secretion system UR - http://hdl.handle.net/10204/5519 ER - en_ZA


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