The [URE3] prion is an aggregated form of Ure2p that can be cured by overexpression of Ure2p fragments
AUTOR(ES)
Edskes, Herman K.
FONTE
The National Academy of Sciences
RESUMO
The [URE3] nonchromosomal genetic element is a prion of Ure2p, a regulator of nitrogen catabolism in Saccharomyces cerevisiae. Ure2p1–65 is the prion domain of Ure2p, sufficient to propagate [URE3] in vivo. We show that full length Ure2p–green fluorescent protein (GFP) or a Ure2p1–65-GFP fusion protein is aggregated in cells carrying [URE3] but is evenly distributed in cells lacking the [URE3] prion. This indicates that [URE3] involves a self-propagating aggregation of Ure2p. Overexpression of Ure2p1–65 induces the de novo appearance of [URE3] by 1,000-fold in a strain initially [ure-o], but cures [URE3] from a strain initially carrying the [URE3] prion. Overexpression of several other fragments of Ure2p or Ure2-GFP fusion proteins also efficiently cures the prion. We suggest that incorporation of fragments or fusion proteins into a putative [URE3] “crystal” of Ure2p poisons its propagation.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=15494Documentos Relacionados
- The mechanisms of [URE3] prion elimination demonstrate that large aggregates of Ure2p are dead-end products
- The yeast prion [URE3] can be greatly induced by a functional mutated URE2 allele
- Conservation of the Prion Properties of Ure2p through Evolution
- Two Prion-Inducing Regions of Ure2p Are Nonoverlapping
- Induction of Distinct [URE3] Yeast Prion Strains
