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Structure of a designed tetrahedral protein assembly variant engineered to have improved soluble expression.


ABSTRACT: We recently reported the development of a computational method for the design of coassembling multicomponent protein nanomaterials. While four such materials were validated at high-resolution by X-ray crystallography, low yield of soluble protein prevented X-ray structure determination of a fifth designed material, T33-09. Here we report the design and crystal structure of T33-31, a variant of T33-09 with improved soluble yield resulting from redesign efforts focused on mutating solvent-exposed side chains to charged amino acids. The structure is found to match the computational design model with atomic-level accuracy, providing further validation of the design approach and demonstrating a simple and potentially general means of improving the yield of designed protein nanomaterials.

SUBMITTER: Bale JB 

PROVIDER: S-EPMC4594668 | biostudies-literature | 2015 Oct

REPOSITORIES: biostudies-literature

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Structure of a designed tetrahedral protein assembly variant engineered to have improved soluble expression.

Bale Jacob B JB   Park Rachel U RU   Liu Yuxi Y   Gonen Shane S   Gonen Tamir T   Cascio Duilio D   King Neil P NP   Yeates Todd O TO   Baker David D  

Protein science : a publication of the Protein Society 20150806 10


We recently reported the development of a computational method for the design of coassembling multicomponent protein nanomaterials. While four such materials were validated at high-resolution by X-ray crystallography, low yield of soluble protein prevented X-ray structure determination of a fifth designed material, T33-09. Here we report the design and crystal structure of T33-31, a variant of T33-09 with improved soluble yield resulting from redesign efforts focused on mutating solvent-exposed  ...[more]

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