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dc.contributor.authorAtarashi, Ryuichirode
dc.contributor.authorKatamine, Shigerude
dc.contributor.authorSakaguchi, Suehirode
dc.contributor.authorShigematsu, Kazutode
dc.date.accessioned2008-06-17T13:46:42Z-
dc.date.available2008-06-17T13:46:42Z-
dc.date.issued2004-10-28de
dc.identifier.issn1611-2156de
dc.identifier.urihttp://hdl.handle.net/2003/25639-
dc.identifier.urihttp://dx.doi.org/10.17877/DE290R-8160-
dc.description.abstractCellular prion protein, PrP^C, undergoes pathogenic structural conversion into the proteinase K (PK)-resistant isoform, PrP^Sc, to constitute a nucleic acid-free infectious agent, so called a prion. To determine whether a recently identified PrP-like protein, named PrPLP/Dpl, could also be transformed to a prion-like protein, we intracerebrally inoculated a mouse-adapted Fukuoka-1 prion into Ngsk and Zrch I mice either homozygously (Prnp^0/0) or heterozygously (Prnp^0/+) devoid of PrP^C. Only the former expressed PrPLP/Dpl ectopically in the brains, particularly in neurons. Ngsk Prnp^0/+ and Zrch I Prnp^0/+ mice similarly developed the disease. The diseased Ngsk Prnp0/+ mice transmitted the disease to the mice expressing PrP^C but not to the mice expressing PrPLP/Dpl, showing abundant accumulation of PrP^Sc but not PK-resistant PrPLP/Dpl in the brains. Moreover, the inoculated Ngsk Prnp^0/0 mice neither developed the disease nor produced any infectivity transmissible to PrPLP/Dpl-expressing mice. These results indicate that PrPLP/Dpl have no potential to undergo pathogenic conversion to form a prion-like infectious particle.en
dc.language.isoende
dc.relation.ispartofseriesEXCLI Journal ; Vol. 3, 2004en
dc.subjectknockout miceen
dc.subjectprionen
dc.subjectprion proteinen
dc.subjectprion protein-like proteinen
dc.subject.ddc610-
dc.titleThe Absence of Prion-Like Infectivity in Mice expressing Prion Protein-Like Proteinen
dc.typeTextde
dc.type.publicationtypearticlede
dcterms.accessRightsopen access-
eldorado.dnb.zdberstkatid2132560-1-
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