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Computational design of a protein family that adopts two well-defined and structurally divergent

biorxiv. 2017; 
Kathy Y. Wei, , Danai Moschidi , Matthew J. Bick, Santrupti Nerli, Andrew C. McShan , Lauren P. Carter , Po-Ssu Huang , Daniel A. Fletcher, , Nikolaos G. Sgourakis , Scott E. Boyken, * , David Baker, ,
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Gene Synthesis Synthetic genes were ordered from Genscript Inc. (Piscataway, NJ, USA) and delivered in pET28b+ E. coli expression vectors, inserted at the NdeI and XhoI sites. Genes are encoded in frame with the N-terminal hexahistidine tag and thrombin cleavage site. A stop codon was added at the C-terminus just before XhoI. Get A Quote

摘要

The plasticity of naturally occurring protein structures, which can change shape considerably in response to changes in environmental conditions, is critical to biological function. While computational methods have been used to de novo design proteins that fold to a single state with a deep free energy minima (Huang et al., 2016), and to reengineer natural proteins to alter their dynamics (Davey et al., 2017) or fold (Alexander et al., 2009), the de novo design of closely related sequences which adopt well-defined, but structurally divergent structures remains an outstanding challenge. Here, we design closely related sequences (over 94% identity) that can adopt two very different homotrimeric helical bundle con... More

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