Team:UCSF/ProjectOverview
From 2011.igem.org
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<regulartext>For our project, we decided to utilize the a-agglutinin half of the aggregation display system to form artificial biofilms. By placing sequences of strong adhesive proteins behind the GPI anchor-Aga1-Aga2 gene and overexpressing them, we were able to create yeast cells that could adhere to different surfaces and even other yeast cells. A couple genes we used to attach to the end of the Aga1p-Aga2p complex were mice cadherins, proteins that mussels used to stick to rocks, and proteins used by other yeast species to initiate biofilm formation. <p></regulartext> | <regulartext>For our project, we decided to utilize the a-agglutinin half of the aggregation display system to form artificial biofilms. By placing sequences of strong adhesive proteins behind the GPI anchor-Aga1-Aga2 gene and overexpressing them, we were able to create yeast cells that could adhere to different surfaces and even other yeast cells. A couple genes we used to attach to the end of the Aga1p-Aga2p complex were mice cadherins, proteins that mussels used to stick to rocks, and proteins used by other yeast species to initiate biofilm formation. <p></regulartext> | ||
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+ | <regulartext1> <b>Interaction of Aga1 with Aga2-fused protein of interest leads to Yeast Cell Surface Display</b> </regulartext1> </div> | ||
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+ | <regulartext1> <b>Interaction of Two Cells via Yeast Cell Surface Display</b> </regulartext1> </div> | ||
Latest revision as of 22:58, 27 September 2011