Team:Dundee

From 2012.igem.org

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       <li class='has-sub '><a href='#'><span>Team</span></a>
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                     <li><a href='https://2012.igem.org/Team:Dundee/Team'><span>Team Members</span></a></li>
                     <li><a href='https://igem.org/Team.cgi?year=2012&team_name=Dundee'><span>iGEM team Profile</span></a></li>
                     <li><a href='https://igem.org/Team.cgi?year=2012&team_name=Dundee'><span>iGEM team Profile</span></a></li>
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Revision as of 22:14, 12 September 2012

Clostridium difficile (C. diff) - associated disease of the gut is a major health problem, and current treatment methods are both ineffective and unpalatable.  Previous research identified a C. diff-specific endolysin from the phage ΦCD27, which could be used to kill C. diff cells. Type VI secretions systems, found in a variety of organisms including Salmonella typhimurium, are characterised by a needle structure, the primary component of which is encoded by the gene Hcp. The tip of the needle is encoded by VgrG. The aim of this project was to create a new type of synthetic Escherichia coli expressing a simplified version of the Type VI Secretion System, with the C. diff-specific endolysin fused to VgrG, and which could be delivered to the gut to combat serious C. diff infections. Mathematical modelling was used to assist in the biological planning and a variety of relevant software applications were made.