Team:Lethbridge/Modeling
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=<font color="white">Homology Modeling= | =<font color="white">Homology Modeling= | ||
- | + | One aspect of our project is working on the localization of catechol-2,3,-dioxygenase (and other proteins) into the interior of <html><a href="https://2010.igem.org/Team:Lethbridge/Project/Compartamentalization"><font color="#00DC00"> microcompartments</font></a></html>. To target the protein into the microcompartment (Lumazine modified to have an even more charged interior) requires the fusion of a polyarginine tail to either the C or N terminus of the protein. | |
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However, these results are from only using one force field and by holding the structure of the rest of the protein static. The use of simulated annealing methods or even molecular dynamics would greatly increase our ability to predict the effect of these tags. | However, these results are from only using one force field and by holding the structure of the rest of the protein static. The use of simulated annealing methods or even molecular dynamics would greatly increase our ability to predict the effect of these tags. | ||
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===<font color="white">References=== | ===<font color="white">References=== | ||
Arnold, K., Bordoli, L., Kopp, J., and Schwede, T. (2006) The SWISS-MODEL Workspace: A web-based environment for protein structure homology modelling., Bioinformatics 22, 195-201. | Arnold, K., Bordoli, L., Kopp, J., and Schwede, T. (2006) The SWISS-MODEL Workspace: A web-based environment for protein structure homology modelling., Bioinformatics 22, 195-201. |