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Microbiol Biotechnol Rep | Volume 1, Issue 2

November 16-17, 2017 Atlanta, Georgia, USA

Annual Congress on

Mycology and Fungal Infections

Aggregate formation by prionogenic proteins in yeast

Anastasia V Grizel

, Aleksandr A Rubel

and

Yury O Chernoff

1,2

St. Petersburg State University, Russia

Georgia Institute of Technology, USA

ross-beta protein polymers (amyloids) cause diseases in mammals and control heritable traits in yeast. Initial

amyloid formation is poorly understood. Amyloid (prion) form of the

Saccharomyces cerevisiae

protein

Sup35 ([

PSI

]) is induced by overproduction of the Sup35 prion domain (PrD) either in the presence of the

prion isoform of another protein (for example, Rnq1), or when Sup35 PrD is attached to another amyloidogenic

protein, e. g. human Abeta peptide. This is accompanied by generation of various types of protein aggregates,

among them filamentous structures representing intermediates of prion formation. We studied if filaments could

be formed by Sup35 PrDs from other yeast species, or by chimeric constructs including both Abeta peptide and a

fluorophore. Divergent Sup35 PrDs from various yeast species, or a chimeric protein composed of

S. cerevisiae

Sup35 PrD and human Abeta were tagged with fluorophores and expressed in the

S. cerevisiae

cells, either

containing ([

PIN

]) or lacking ([

pin

]) the Rnq1 prion. Sup35 PrDs from various yeast species differed from

each other by morphology of aggregates formed in the [

PIN

] cells. Some divergent proteins produced almost no

filaments, although this did not necessarily correlate with the evolutionary distance. The Sup35 PrD-Abeta-CFP

construct rapidly and efficiently formed dot-like aggregates in the [

pin

] cells. However, this aggregation

did not result in [

PSI

] induction, indicating that either prion formation or immobilization of full size sup35

into a prion is inhibited by the attachment of fluorophore to the C-terminus of Abeta. Supported by SPbSU

grant 1.50.1038.2014, RFBR 15-04-06650 and RSF 14-50-00069.

Biography

Anastasia V Grizel has received her PhD in Biophysics from Lomonosov Moscow State University in 2012, and performed postdoctoral studies at St. Petersburg

State University. She currently is a Research Scientist at St. Petersburg State University (Russia). Her area of research includes genetic, cytological and structural

analysis of protein aggregation, primarily in the yeast model. She has published six papers in scientific journals.

avgrizel@gmail.com