Prion Domain Initiation of Amyloid Formation in Vitro from Native Ure2p

Kimberly L. Taylor; Naiqian Cheng; Robert W. Williams; Alasdair C. Steven; Reed B. Wickner

doi:10.1126/science.283.5406.1339

Prion Domain Initiation of Amyloid Formation in Vitro from Native Ure2p

Kimberly L. Taylor(National Institute of Diabetes and Digestive and Kidney Diseases), Naiqian Cheng(National Institute of Arthritis and Musculoskeletal and Skin Diseases), Robert W. Williams(Uniformed Services University of the Health Sciences), Alasdair C. Steven(National Institute of Arthritis and Musculoskeletal and Skin Diseases), Reed B. Wickner(National Institute of Diabetes and Digestive and Kidney Diseases)

Science

February 26, 1999

10.1126/science.283.5406.1339

Cited by 278

Abstract

The [URE3] non-Mendelian genetic element of Saccharomyces cerevisiae is an infectious protein (prion) form of Ure2p, a regulator of nitrogen catabolism. Here, synthetic Ure2p1-65 were shown to polymerize to form filaments 40 to 45 angstroms in diameter with more than 60 percent beta sheet. Ure2p1-65 specifically induced full-length native Ure2p to copolymerize under conditions where native Ure2p alone did not polymerize. Like Ure2p in extracts of [URE3] strains, these 180- to 220-angstrom-diameter filaments were protease resistant. The Ure2p1-65-Ure2p cofilaments could seed polymerization of native Ure2p to form thicker, less regular filaments. All filaments stained with Congo Red to produce the green birefringence typical of amyloid. This self-propagating amyloid formation can explain the properties of [URE3].

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