Optimizing protein stability in vivo.

نویسندگان

  • Linda Foit
  • Gareth J Morgan
  • Maximilian J Kern
  • Lenz R Steimer
  • Annekathrin A von Hacht
  • James Titchmarsh
  • Stuart L Warriner
  • Sheena E Radford
  • James C A Bardwell
چکیده

Identifying mutations that stabilize proteins is challenging because most substitutions are destabilizing. In addition to being of immense practical utility, the ability to evolve protein stability in vivo may indicate how evolution has formed today's protein sequences. Here we describe a genetic selection that directly links the in vivo stability of proteins to antibiotic resistance. It allows the identification of stabilizing mutations within proteins. The large majority of mutants selected for improved antibiotic resistance are stabilized both thermodynamically and kinetically, indicating that similar principles govern stability in vivo and in vitro. The approach requires no prior structural or functional knowledge and allows selection for stability without a need to maintain function. Mutations that enhance thermodynamic stability of the protein Im7 map overwhelmingly to surface residues involved in binding to colicin E7, showing how the evolutionary pressures that drive Im7-E7 complex formation have compromised the stability of the isolated Im7 protein.

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عنوان ژورنال:
  • Molecular cell

دوره 36 5  شماره 

صفحات  -

تاریخ انتشار 2009