A prion protein epitope selective for the pathologically misfolded conformation

被引:0
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作者
Eustache Paramithiotis
Marc Pinard
Trebor Lawton
Sylvie LaBoissiere
Valerie L Leathers
Wen-Quan Zou
Lisa A Estey
Julie Lamontagne
Marty T Lehto
Leslie H Kondejewski
Gregory P Francoeur
Maria Papadopoulos
Ashkan Haghighat
Stephen J Spatz
Mark Head
Robert Will
James Ironside
Katherine O'Rourke
Quentin Tonelli
Harry C Ledebur
Avi Chakrabartty
Neil R Cashman
机构
[1] Caprion Pharmaceuticals Inc.,Department of Medical Biophysics
[2] IDEXX Laboratories Inc.,undefined
[3] The National Creutzfeldt-Jakob Disease Surveillance Unit,undefined
[4] Western General Hospital,undefined
[5] USDA-ARS-ADRU,undefined
[6] 3003 ADBF,undefined
[7] Washington State University,undefined
[8] University of Toronto,undefined
[9] Ontario Cancer Institute,undefined
[10] Centre for Research in Neurodegenerative Diseases,undefined
[11] 6 Queen's Park Crescent West,undefined
[12] University of Toronto,undefined
[13] Sunnybrook & Women's College Health Sciences Centre,undefined
[14] University of Toronto,undefined
[15] Vertex Inc.,undefined
来源
Nature Medicine | 2003年 / 9卷
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摘要
Conformational conversion of proteins in disease is likely to be accompanied by molecular surface exposure of previously sequestered amino-acid side chains. We found that induction of β-sheet structures in recombinant prion proteins is associated with increased solvent accessibility of tyrosine. Antibodies directed against the prion protein repeat motif, tyrosine-tyrosine-arginine, recognize the pathological isoform of the prion protein but not the normal cellular isoform, as assessed by immunoprecipitation, plate capture immunoassay and flow cytometry. Antibody binding to the pathological epitope is saturable and specific, and can be created in vitro by partial denaturation of normal brain prion protein. Conformation-selective exposure of Tyr-Tyr-Arg provides a probe for the distribution and structure of pathologically misfolded prion protein, and may lead to new diagnostics and therapeutics for prion diseases.
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页码:893 / 899
页数:6
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