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The Schizosaccharomyces pombe Hsp104 disaggregase is unable to propagate the [PSI] prion.

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TLDR
It is demonstrated that the ability to untangle aggregated proteins is conserved between the S. pombe and S. cerevisiae Hsp104 homologs, and points to a role of the CTD in the propagation ofThe S. Cerevisiae [PSI+] prion.
Abstract
The molecular chaperone Hsp104 is a crucial factor in the acquisition of thermotolerance in yeast. Under stress conditions, the disaggregase activity of Hsp104 facilitates the reactivation of misfolded proteins. Hsp104 is also involved in the propagation of fungal prions. For instance, the well-characterized [PSI+] prion of Saccharomyces cerevisiae does not propagate in Δhsp104 cells or in cells overexpressing Hsp104. In this study, we characterized the functional homolog of Hsp104 from Schizosaccharomyces pombe (Sp_Hsp104). As its S. cerevisiae counterpart, Sp_hsp104+ is heat-inducible and required for thermotolerance in S. pombe. Sp_Hsp104 displays low disaggregase activity and cannot propagate the [PSI+] prion in S. cerevisiae. When overexpressed in S. cerevisiae, Sp_Hsp104 confers thermotolerance to Δhsp104 cells and reactivates heat-aggregated proteins. However, overexpression of Sp_Hsp104 does not propagate nor eliminate [PSI+]. Strikingly, [PSI+] was cured by overexpression of a chimeric chaperone bearing the C-terminal domain (CTD) of the S. cerevisiae Hsp104 protein. Our study demonstrates that the ability to untangle aggregated proteins is conserved between the S. pombe and S. cerevisiae Hsp104 homologs, and points to a role of the CTD in the propagation of the S. cerevisiae [PSI+] prion.

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Journal ArticleDOI

Prions in Yeast

TL;DR: This review summarizes what has been learned from yeast prions and continues to lead the way in understanding cellular control of prion propagation, prion structure, mechanisms of de novo prion formation, specificity ofPrion transmission, and the biological roles of prions.
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Prions, protein homeostasis, and phenotypic diversity

TL;DR: It is suggested that these qualities allow prions to act as 'bet-hedging' devices that facilitate the adaptation of yeasts to stressful environments, and might speed the evolution of new traits.
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Fission Yeast Does Not Age under Favorable Conditions, but Does So after Stress

TL;DR: It is concluded that S. pombe does not age under favorable growth conditions, but does so under stress, and this transition appears to be passive rather than active and results from the formation of a single large aggregate, which segregates asymmetrically at the subsequent cell division.
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The elusive middle domain of Hsp104 and ClpB: Location and function

TL;DR: Recent advances have illuminated that the MD is critical for the intrinsic disaggregase activity of the hexamer and mediates key functional interactions with the Hsp70 chaperone system that empower protein disaggregation.
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Insight into molecular basis of curing of [PSI+] prion by overexpression of 104-kDa heat shock protein (Hsp104).

TL;DR: Understanding the molecular basis of prion remodeling by Hsp104 may have implications for understanding how protein aggregation associated with disease could be mitigated by molecular chaperones, and sheds light on the limitations of the ability of Hsp 104 to eliminate aggregates produced by other aggregation-prone proteins.
References
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