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Original Article |
BACKGROUND: The [PSI+] element of the budding yeast is an aggregated form of the translation release factor Sup35 that is propagated and transmitted cytoplasmically in a manner analogous to that of mammalian prions. The N-terminal of Sup35, necessary for [PSI+], contains oligopeptide repeats and multiple Gln/Asn residues. RESULTS: We replaced the Gln/Asn-rich prion repeats of Sup35 with non-Gln/Asn repeats from heterologous yeast strains. These non-Gln/Asn repeat Sup35s propagated a novel [PSI+] variant, [PHI+], that appeared de novo 103 times more frequent than [PSI+]. [PHI+] was stably inherited in a non-Mendelian fashion, but not eliminated upon the inactivation of Hsp104, unlike known [PSI+] elements. In vitro, non-Gln/Asn repeat domains formed amyloid fibres that were shorter and grew more slowly than did Gln/Asn-rich prion domains, while [PHI+] aggregates were smaller than [PSI+] aggregates in vivo. CONCLUSIONS: These findings suggest the existence of an alternative, Hsp104-independent pathway to replicate non-Gln/Asn variant Sup35 prion seeds.
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 P. Collin, P. B. Beauregard, A. Elagoz, and L. A. Rokeach A non-chromosomal factor allows viability of Schizosaccharomyces pombe lacking the essential chaperone calnexin J. Cell Sci., February 22, 2004; 117(6): 907 - 918. [Abstract] [Full Text] [PDF]
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 D. S. Kryndushkin, I. M. Alexandrov, M. D. Ter-Avanesyan, and V. V. Kushnirov Yeast [PSI+] Prion Aggregates Are Formed by Small Sup35 Polymers Fragmented by Hsp104 J. Biol. Chem., December 5, 2003; 278(49): 49636 - 49643. [Abstract] [Full Text] [PDF]
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