Team:Freiburg/Modelling

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(Difference between revisions)
(Modelling: Rational protein design)
(Modelling: Rational protein design)
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After combining these caps with our structural analysis for possible Nickel binding sites and filling the empty positions of the consensus sequence with the ideal sequence derived from the ligase sequence(see above), we were still unsure whether this would work out. To increase our chances of success we designed six different versions with distinct Histidine patterns on the LRR core.
After combining these caps with our structural analysis for possible Nickel binding sites and filling the empty positions of the consensus sequence with the ideal sequence derived from the ligase sequence(see above), we were still unsure whether this would work out. To increase our chances of success we designed six different versions with distinct Histidine patterns on the LRR core.
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{|style="color:black; border="1" width="85%"
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;[[File:Freiburg11_Seq6.png|750px]]
;[[File:Freiburg11_Seq6.png|750px]]
|}
|}
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Revision as of 16:44, 20 September 2011


This is the wiki page
of the Freiburger student
team competing for iGEM 2011.
Thank you for your interest!