Some prion protein mutations create anchorless molecules that cause Gerstmann–Sträussler–Scheinker (GSS) disease. To model GSS, we generated transgenic mice expressing cellular prion protein (PrPC) lacking the glycosylphosphatidyl inositol (GPI) anchor, denoted PrP(ΔGPI). Mice overexpressing PrP(ΔGPI) developed a late-onset, spontaneous neurologic dysfunction characterized by widespread amyloid deposition in the brain and the presence of a short protease-resistant PrP fragment similar to those found in GSS patients. In Tg(PrP,ΔGPI) mice, disease onset could be accelerated either by inoculation with brain homogenate prepared from spontaneously ill animals or by coexpression of membrane-anchored, full-length PrPC. In contrast, coexpression of N-terminally truncated PrP(Δ23–88) did not affect disease progression. Remarkably, disease from ill Tg(PrP,ΔGPI) mice transmitted to mice expressing wild-type PrPC, indicating the spontaneous generation of prions.
|Titolo:||Spontaneous generation of anchorless prions in transgenic mice|
|Autori:||Stöhr, J; Watts, Jc; Legname, Giuseppe; Oehler, A; Lemus, A; Nguyen, Ho; Sussman, J; Wille, H; Dearmond, Sj; Prusiner, Sb; Giles, K.|
|Data di pubblicazione:||2011|
|Digital Object Identifier (DOI):||10.1073/pnas.1117827108|
|Appare nelle tipologie:||1.1 Journal article|