Protease-sensitive Scrapie Prion Protein in Aggregates of Heterogeneous Sizes

Overview

Journal Biochemistry

Specialty Biochemistry

Date 2002 Oct 16

PMID 12379130

Citations 108

Authors

Salit Tzaban

Gilgi Friedlander

Oshrat Schonberger

Lior Horonchik

Yifat Yedidia

Gideon Shaked

Ruth Gabizon

Albert Taraboulos

Affiliations

Soon will be listed here.

Abstract

The pathological prion protein PrP(Sc) is the only known component of the infectious prion. In cells infected with prions, PrP(Sc) is formed posttranslationally by the refolding of the benign cell surface glycoprotein PrP(C) into an aberrant conformation. The two PrP isoforms possess very different properties, as PrP(Sc) has a protease-resistant core, forms very large amyloidic aggregates in detergents, and is only weakly immunoreactive in its native form. We now show that prion-infected rodent brains and cultured cells contain previously unrecognized protease-sensitive PrP(Sc) varieties. In both ionic (Sarkosyl) and nonionic (n-octyl beta-D-glucopyranoside) detergents, the novel protease-sensitive PrP(Sc) species formed aggregates as small as 600 kDa, as measured by gel filtration. The denaturation dependence of PrP(Sc) immunoreactivity correlated with the size of the aggregate. The small PrP(Sc) aggregates described here are consistent with the previous demonstration of scrapie infectivity in brain fractions with a sedimentation coefficient as small as 40 S [Prusiner et al. (1980) J. Neurochem. 35, 574-582]. Our results demonstrate for the first time that prion-infected tissues contain protease-sensitive PrP(Sc) molecules that form low MW aggregates. Whether these new PrP(Sc) species play a role in the biogenesis or the pathogenesis of prions remains to be established.

Citing Articles

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Asymmetric-flow field-flow fractionation of prions reveals a strain-specific continuum of quaternary structures with protease resistance developing at a hydrodynamic radius of 15 nm.

Cortez L, Nemani S, Duque Velasquez C, Sriraman A, Wang Y, Wille H PLoS Pathog. 2021; 17(6):e1009703.

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