[PIN+]: prions beget prions

Liebman, Susan

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Introduction
Prion paradigm in yeast
Hsp104 chaperone required for prions propagation
Amyloid-like prion proteins in yeast
[psi -] vs. [PSI +] cells
Some genetic criteria suggestive of prions (1)
Some genetic criteria suggestive of prions (2)
Sup35 protein structure
Different variants of [PSI +]
Dominant prios compete better for soluble protein
Variant differences are prion specific
[PIN +] causes [PSI +] induction
Excess Sup35 inhibit growth of [PIN +] cells
[PIN +] phenotypes
Genetics of [PIN +] (1)
[PIN +] maintenance is independent of [PSI +] PD
[PSI +] and [PIN +] can be lost independently
Prions do not protect each other from being cured
Genetics of [PIN +] (2)
Reversible curing of [PIN +]
Genetics of [PIN +] (3)
Different variants of [PIN +]
[PIN +] "Variants" are transferred by cytoduction
[PSI +] phenotypes are not affected by [PIN +]
[PIN +] effect on SDS resistant [PSI +] oligomers
Some [PIN +] variants destabilize weak [PSI +]
[PIN +] enhances the appearance of [URE3]
[PIN +] enhances aggregation of polyQ
Extensions affect [PIN +] dependence
Candidate approach to identify the [PIN +] gene
RNQ1 is required for [PIN +] propagation
Rnq1 sedimentation in different [PIN +]'s
Rnq1
RNQ1-PD amyloid aggregates transmit [PIN+]
[PIN +] and [PSI +] oligomers are distinct
Pin+ is not caused by loss of Rnq1 function
Models for [PSI +] appearance induction
RNQ1 aggregates stimulate NM fiber formation
NM fibers stimulate RNQ1-PD aggregate formation
Can other prions cross-seed [PSI +] formation?
Eleven QN-rich potential prions cloned
Other prions enhance de novo [PSI +] appearance
URE3 enhances Rnq1:GFP aggregate appearance
Genes enhance Rnq1:GFP aggregate appearance
Q103:GFP aggregates enhance PSI+ appearance
Conclusions
Acknowledgements
Collaborators
References

Topics Covered

Prions are infectious proteins
[PIN+] is a prion of Rnq1
[PIN+] exists as different variants
Prions can affect the stability of other variants of the same prion, or of heterologous prions

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Prions and Amyloids

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Talk Citation

Liebman, S. (2020, May 1). [PIN+]: prions beget prions [Video file]. In The Biomedical & Life Sciences Collection, Henry Stewart Talks. Retrieved November 23, 2024, from https://doi.org/10.69645/OIPW1902.
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Publication History

Published on September 4, 2008
Reviewed on May 1, 2020
Archived on February 25, 2021

Financial Disclosures

Prof. Susan Liebman has not informed HSTalks of any commercial/financial relationship that it is appropriate to disclose.

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[PIN+]: prions beget prions

Prof. Susan Liebman – University of Illinois at Chicago, USA

Published on September 4, 2008 Archived on February 25, 2021 42 min

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Transcript

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0:00

In this seminar, I will tell you how the presence of one yeast prion can enhance the appearance of other yeast prions.

0:09

According to the prion paradigm in yeast cells can propagate prion proteins in either the normal form or the prion form. When propagated in the prion form, they have a different phenotype than in cultures where the protein is propagated and the normal form. Cells with the prion in the normal form can be converted into prion cultures by being infected with prion seed. Evidence suggests that the prion seed is a fiber and that the normal molecules join this fiber at the ends.

0:46

The growth of the prion fiber is limited by the fact that it only has two ends. And as you could imagine, its ability to segregate into budding daughter cells is also limited by the number of prion seeds that are present in the mother. The Hsp104 chaperone whose activity is known to disaggregate aggregated proteins provides the important activity for the prion of cutting these fibers into pieces, which provides additional ends and additional seeds that can then segregate into the daughters. In the absence of Hsp104 of course, the prions are not cut and they fail to segregate and are lost, leading to the curing of cells of the prion. This also explains how the low levels of guanidine hydrochloride, known for many years to cure cells of prions works and it does so we now know by inhibiting the activity of the Hsp104 chaperone.

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[PIN+]: prions beget prions

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[PIN+]: prions beget prions