1. Detection of misfolded prion protein in blood with conformationally sensitive peptides.
- Author
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Tao Pan, Sethi, Jasmeet, Nelsen, Craig, Rudolph, Alan, Cervenakova, Larisa, Brown, Paul, and Orser, Cindy S.
- Subjects
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BLOOD proteins , *PEPTIDES , *CHRONIC wasting disease , *PRION diseases , *SERUM , *BLOOD plasma - Abstract
BACKGROUND: The long-standing goal of a preclinical diagnostic test for transmissible spongiform encephalopathy (TSE) has recently become urgent because of the discovery that humans with variant Creutzfeldt-Jakob disease can transmit disease via blood transfusions. STUDY DESIGN AND METHODS: The misfolded protein diagnostic (MPD) assay employs a pyrene-labeled palindromic sequence of prion peptides that undergoes a cascade of coil to β-sheet conversion in the presence of the misfolded prion protein (PrPTSE). The ability of the assay to detect PrPTSE in brain, serum, and plasma was tested. The basic protocol involved a several-hour incubation of 200-µL sample volumes with the peptide reagent in 96-well plates, after which fluorescence was monitored by a fluorescence plate reader with an excitation wavelength of 350 nm and emission scanning wavelength range of 365 to 600 nm. RESULTS: Target specificity for PrPTSE was documented by correlation of assay signal with Western blot signals in brain tissue from TSE-infected, normal, and knockout mice and negative assay signals by use of reagents with different peptide sequences. When applied to plasma or serum, the assay discriminated between samples from a variety of experimental and natural TSE infections compared to uninfected controls, with a sensitivity threshold of approximately 1 infectious dose per mL in pooled plasma from TSE-infected mice. CONCLUSIONS: The MPD assay is a sensitive and specific test for the detection of PrPTSE that may be useful in both preclinical and clinical diagnosis of TSE diseases of animals and humans. [ABSTRACT FROM AUTHOR]
- Published
- 2007
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