Neuroreport. 2007 Dec 3;18(18):1935-8.

Elk with a long incubation prion disease phenotype have a unique PrPd profile.

O'Rourke KI, Spraker TR, Zhuang D, Greenlee JJ, Gidlewski TE, Hamir AN.

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United States Department of Agriculture, Agricultural Research Service, Animal Disease Research Unit, Pullman, Washington 99164, USA. karourke@vetmed.wsu.edu

Abstract

The transmissible spongiform encephalopathies (TSEs) invariably result in fatal neurodegeneration and accumulation of PrP, an abnormal form of the host prion protein PrP, encoded by the PRNP gene. A naturally occurring polymorphism (methionine/valine) at PRNP codon 129 is associated with variation in relative disease susceptibility, incubation time, clinical presentation, neuropathology, and/or PrP biochemical characteristics in a range of human TSEs. A methionine/leucine polymorphism at the corresponding site in the Rocky Mountain elk PRNP gene is associated with variation in relative susceptibility and incubation time in the cervid TSE chronic wasting disease. We now report that elk lacking the predisposing 132-methionine allele develop chronic wasting disease after a long incubation period and display a novel PrP folding pattern.

PMID:: 18007190; [PubMed - indexed for MEDLINE]

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Elk with a long incubation prion disease phenotype have a unique PrPd profile.
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Elk with a long incubation prion disease phenotype have a unique PrPd profile.

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