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Structural Basis for Modulation of Quality Control Fate in a Marginally Stable Protein.


ABSTRACT: The human von Hippel-Lindau (VHL) tumor suppressor is a marginally stable protein previously used as a model substrate of eukaryotic refolding and degradation pathways. When expressed in the absence of its cofactors, VHL cannot fold and is quickly degraded by the quality control machinery of the cell. We combined computational methods with in vivo experiments to examine the basis of the misfolding propensity of VHL. By expressing a set of randomly mutated VHL sequences in yeast, we discovered a more stable mutant form. Subsequent modeling suggested the mutation had caused a conformational change affecting cofactor and chaperone interaction, and this hypothesis was then confirmed by additional knockout and overexpression experiments targeting a yeast cofactor homolog. These findings offer a detailed structural basis for the modulation of quality control fate in a model misfolded protein and highlight burial mode modeling as a rapid means to detect functionally important conformational changes in marginally stable globular domains.

SUBMITTER: Brock KP 

PROVIDER: S-EPMC4509718 | biostudies-literature | 2015 Jul

REPOSITORIES: biostudies-literature

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Structural Basis for Modulation of Quality Control Fate in a Marginally Stable Protein.

Brock Kelly P KP   Abraham Ayelet-chen AC   Amen Triana T   Kaganovich Daniel D   England Jeremy L JL  

Structure (London, England : 1993) 20150528 7


The human von Hippel-Lindau (VHL) tumor suppressor is a marginally stable protein previously used as a model substrate of eukaryotic refolding and degradation pathways. When expressed in the absence of its cofactors, VHL cannot fold and is quickly degraded by the quality control machinery of the cell. We combined computational methods with in vivo experiments to examine the basis of the misfolding propensity of VHL. By expressing a set of randomly mutated VHL sequences in yeast, we discovered a  ...[more]

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