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De novo design of a fluorescence-activating β-barrel.

Nature. 2018; 
Dou J,, Vorobieva AA,, Sheffler W,, Doyle LA, Park H,, Bick MJ,, Mao B,, Foight GW, Lee MY, Gagnon LA, Carter L,, Sankaran B, Ovchinnikov S,,, Marcos E,,, Huang PS,,, Vaughan JC, Stoddard BL, Baker D,,.
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Custom Vector Construction Genes encoding the non-functional β-barrel designs (41 from parametric design and 4 from fragment-base design) were syn- thesized and cloned into the pET-29 vector (GenScript). Get A Quote

摘要

The regular arrangements of β-strands around a central axis in β-barrels and of α-helices in coiled coils contrast with the irregular tertiary structures of most globular proteins, and have fascinated structural biologists since they were first discovered. Simple parametric models have been used to design a wide range of α-helical coiled-coil structures, but to date there has been no success with β-barrels. Here we show that accurate de novo design of β-barrels requires considerable symmetry-breaking to achieve continuous hydrogen-bond connectivity and eliminate backbone strain. We then build ensembles of β-barrel backbone models with cavity shapes that match the fluorogenic compound DFHBI, and use a hi... More

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