Literature DB >> 26517888

The αRep artificial repeat protein scaffold: a new tool for crystallization and live cell applications.

Marie Valerio-Lepiniec1, Agathe Urvoas1, Anne Chevrel1, Asma Guellouz1, Yann Ferrandez1, Agnès Mesneau1, Ines Li de la Sierra-Gallay1, Magali Aumont-Nicaise1, Michel Desmadril1, Herman van Tilbeurgh1, Philippe Minard2.   

Abstract

We have designed a new family of artificial proteins, named αRep, based on HEAT (acronym for Huntingtin, elongation factor 3 (EF3), protein pphosphatase 2A (PP2A), yeast kinase Tor1) repeat proteins containing an α-helical repeated motif. The sequence of the repeated motifs, first identified in a thermostable archae protein was optimized using a consensus design strategy and used for the construction of a library of artificial proteins. All proteins from this library share the same general fold but differ both in the number of repeats and in five highly randomized amino acid positions within each repeat. The randomized side chains altogether provide a hypervariable surface on αRep variants. Sequences from this library are efficiently expressed as soluble, folded and very stable proteins. αRep binders with high affinity for various protein targets were selected by phage display. Low micromolar to nanomolar dissociation constants between partners were measured and the structures of several complexes (specific αRep/protein target) were solved by X-ray crystallography. Using GFP as a model target, it was demonstrated that αReps can be used as bait in pull-down experiments. αReps can be expressed in eukaryotic cells and specifically interact with their target addressed to different cell compartments.
© 2015 Authors; published by Portland Press Limited.

Entities:  

Keywords:  combinatorial library; crystal structure; protein design; repeat protein; αRep

Mesh:

Substances:

Year:  2015        PMID: 26517888     DOI: 10.1042/BST20150075

Source DB:  PubMed          Journal:  Biochem Soc Trans        ISSN: 0300-5127            Impact factor:   5.407


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