Prions are proteins that self-propagate an aggregated or amyloid-like structure that converts protein from its native state to this aggregated conformation. Proteins that contribute to protein misfolding disorders, like amyloid-2 in Alzheimer's disease, are now thought to misfold and aggregate in a prion-like fashion. When the mammalian prion protein, PrP, adopts its prion conformation (PrPSc), it forms an infectious amyloid that causes fatal neurodegenerative disorders called transmissible spongiform encephalopathies. Different conformations of PrPSc, referred to as prion strains, may be the underlying cause of both the """"""""species barrier"""""""" as well as much of the variation in disease latency and pathology seen in prion diseases. Pathologic variation is also seen in other neurodegenerative disorders, suggesting distinct protein conformations may be involved in these diseases as well. Yet, it is still unclear how different self-propagating structures can originate from one polypeptide. Precisely how prion strains arise de novo and how a single prion protein can acquire and propagate different conformations is entirely unknown. The investigation of prions endogenous to the yeast Saccharomyces cerevisiae has provided much information about the structural differences possible among mammalian prion strains (called variants in yeast). The yeast translation termination factor Sup35p aggregates to form the [PSI+] prion. [PSI+] is an epigenetic factor that has many phenotypic consequences as it globally impacts translation and may be involved in regulating how a cell responds to fluctuating environments. Interestingly, the spontaneous conversion of [PSI+] requires the presence of another prion, [RNQ+], formed by Rnq1p. Both of these prions form different variants that can easily be monitored in the yeast cell. This allows us to examine what factors play a role in dictating how a protein can adopt distinct self-propagating conformations. The following specific aims will use an integrated molecular, genetic, and biochemical approach to investigate how different protein conformations could contribute to both the formation and phenotypic variation of age-related diseases: 1) Determine how [RNQ+] variants facilitate the formation of [PSI+];2) (A) Elucidate intragenic and extragenic mechanisms that regulate the formation and propagation of [RNQ+] variants;(B) Elucidate the key biochemical properties that define prion variants. Overall, this proposal will enhance our understanding of the physical and molecular basis of prion variants and provide insight into how alternative protein conformations can impact transmissibility between species and cause variation in disease progression of neurodegenerative disorders.

Public Health Relevance

Transmissible spongiform encephalopathies (TSEs) are a group of fatal neurodegenerative diseases caused by an infectious conformation of the mammalian prion protein, PrP. These prion diseases received worldwide attention during the outbreak of """"""""mad cow disease"""""""" in the 1990s when it was transmitted from cattle to humans. There is a tremendous amount of pathologic variability seen in TSEs as well as other neurodegenerative disorders, such as Alzheimer's disease. This proposal explores mechanisms to explain how changes in protein conformation can develop and cause this variation. This information will help us understand the progression of these diseases and aid in the search for therapies.

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Predoctoral Individual National Research Service Award (F31)
Project #
1F31AG040899-01
Application #
8201428
Study Section
Special Emphasis Panel (ZRG1-F05-A (20))
Program Officer
Mackiewicz, Miroslaw
Project Start
2011-09-26
Project End
2013-09-25
Budget Start
2011-09-26
Budget End
2012-09-25
Support Year
1
Fiscal Year
2011
Total Cost
$27,977
Indirect Cost
Name
Washington University
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
068552207
City
Saint Louis
State
MO
Country
United States
Zip Code
63130
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Stein, Kevin C; Bengoechea, Rocio; Harms, Matthew B et al. (2014) Myopathy-causing mutations in an HSP40 chaperone disrupt processing of specific client conformers. J Biol Chem 289:21120-30
Stein, Kevin C; True, Heather L (2014) Structural variants of yeast prions show conformer-specific requirements for chaperone activity. Mol Microbiol 93:1156-71
Stein, Kevin C; True, Heather L (2014) Prion strains and amyloid polymorphism influence phenotypic variation. PLoS Pathog 10:e1004328
Stein, Kevin C; True, Heather L (2014) Extensive diversity of prion strains is defined by differential chaperone interactions and distinct amyloidogenic regions. PLoS Genet 10:e1004337
Huang, Vincent J; Stein, Kevin C; True, Heather L (2013) Spontaneous variants of the [RNQ+] prion in yeast demonstrate the extensive conformational diversity possible with prion proteins. PLoS One 8:e79582
Stein, Kevin C; True, Heather L (2011) The [RNQ+] prion: a model of both functional and pathological amyloid. Prion 5:291-8