Team:Potsdam Bioware
From 2011.igem.org
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+ | <img src="https://static.igem.org/mediawiki/2011/0/0e/UP_Nadja.jpg" alt="Nadja Bjelopoljak" /> | ||
+ | <p>Nadja Bjelopoljak</p> | ||
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+ | <img src="https://static.igem.org/mediawiki/2011/e/e4/UP_Nadine.jpg" alt="Nadine Boehmer" /> | ||
+ | <p>Nadine Boehmer</p> | ||
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+ | <img src="https://static.igem.org/mediawiki/2011/8/82/UP_VanessaB.jpg" alt="Vanessa Boehmer" /> | ||
+ | <p>Vanessa Boehmer</p> | ||
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+ | <img src="https://static.igem.org/mediawiki/2011/a/a3/UP_Jessica.jpg" alt="Jessica Eger" /> | ||
+ | <p>Jessica Eger</p> | ||
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+ | <img src="https://static.igem.org/mediawiki/2011/b/b1/UP_Steffi.jpg" alt="Steffi Sempert" /> | ||
+ | <p>Steffi Sempert</p> | ||
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Revision as of 13:46, 18 September 2011
Project
One key task of biopharmaceuticals is the binding and blocking of deregulated proteins. Towards this goal, we mutate and select microviridins, which are tricyclic depsipeptides from cyanobacteria. They are small but stable due to their post-translational side-chain crosslinking. Microviridins have a high potential for therapy as they can block disease-relevant proteases. Yet, the possibilities of cyclic peptides are largely untapped since genetic systems for optimization are not well established. Thus, we developed synthetic systems for the mutation, selection and production of such peptides. We use the 6.5 kb microviridin (mdn) gene cluster cloned in E. coli plasmids, established random mutagenesis and generated focused libraries of microviridins. For selection against a panel of proteases, we are applying and testing phage display, and we are constructing a novel in-vivo selection device, which links protease blocking to antibiotic resistance. Our systems, including the 6.5 kb cluster, adhere to the BioBrick standards.
Software
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Team
Nicole Albrecht
Katharina Berger
Nadja Bjelopoljak
Nadine Boehmer
Vanessa Boehmer
Jessica Eger
Steffi Sempert
BioBricks
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Human Practice
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Labjournal
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Modelling
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