Open Access: CC-BY SHERPA RoMEO: blue
Zgłaszanie prac wstrzymane - Submissions stopped
Tom 13, Nr 4. Zima 2017
Tom 13, Nr 3. Jesień 2017
Tom 13, Nr 2. Lato 2017
Tom 13, Nr 1. Wiosna 2017
Tom 12, Nr 4. Zima 2016
Tom 12, Nr 3. Jesień 2016
Tom 12, Nr 2. Lato 2016
Tom 12, Nr 1. Wiosna 2016
Tom 11, Nr 4. Zima 2015.
Tom 11, Nr 3. Jesień 2015.
Tom 11, Nr 2. Lato 2015
Tom 11, Nr 1. Wiosna 2015
Tom 10, Nr 4. Zima 2014
Tom 10, Nr 3. Jesień 2014
Tom 10, Nr 2. Lato 2014. SUPLEMENT
Tom 10, Nr 2. Lato 2014
Tom 10, Nr 1. Wiosna 2014
Tom 9, Nr 4. Zima 2013
Tom 9, Nr 3. Jesień 2013
Tom 9, Nr 2. Lato 2013
Tom 9, Nr 1. Wiosna 2013
Tom 8, Nr 3-4. Jesień-Zima 2012
Tom 8, Nr 1-2. Wiosna-Lato 2012
Tom 7, Nr 4. Zima 2011
Tom 7, Nr 2-3. Lato-Jesień 2011
Tom 7, Nr 2-3. Lato-Jesień 2011. SUPLEMENT
Tom 7, Nr 1. Wiosna 2011
Tom 6, Nr 3-4. Jesień-Zima 2010
Tom 6, Nr 2. Lato 2010
Tom 6, Nr 1. Wiosna 2010
Tom 5, Nr 3-4. Jesień-Zima 2009
Tom 5, Nr 1-2. Wiosna-Lato 2009
Tom 4, Nr 4. Zima 2008
Tom 4, Nr 2-3. Lato-Jesień 2008
Tom 4, Nr 1. Wiosna 2008
Tom 3, Nr 4. Zima 2007
Tom 3, Nr 3. Jesień 2007
Tom 3, Nr 2. Lato 2007
Tom 3, Nr 1. Wiosna 2007
Tom 2, Nr 4. Zima 2006
Tom 2, Nr 3. Jesień 2006
Tom 2, Nr 3. Jesień 2006, Supl.
Tom 2, Nr 2. Lato 2006
Tom 2, Nr 1. Wiosna 2006
Tom 1, Nr 2. Zima 2005
Tom 1, Nr 1. Jesień 2005.
REGULAMIN OGŁASZANIA PRAC
Redakcja Czasopisma
LISTA RECENZENTÓW CZASOPISMA

Aktualności i opinie

Wyszukiwarka








..:: Choroba Creutzfeldta-Jakoba i inne pasażowalne encefalopatie gąbczaste człowieka. Część II 297 ::..
Choroba Creutzfeldta-Jakoba i inne pasażowalne encefalopatie gąbczaste człowieka. Część II 297
 
Adam Zaborowski
Choroba Creutzfeldta-Jakoba i inne pasażowalne encefalopatie gąbczaste człowieka. Część II       297
Summary The second part of this work presents the neuropathological problems of the Creutzfeldt-Jakob disease and basic informations about other human prion diseases. General problems of prion diseases and clinical symptoms of Creutzfeldt-Jakob disease were presented in the first part. Prion diseases are also known as transmissible cerebral amyloidoses (TCA) or transmissible (subacute) spongiform encephalopathies (TSE, SSE). There are following human TSE's: Creutzfeldt-Jakob disease (CJD) - the most frequent TSE, and its new variant (vCJD) - a result of BSE's transmission into human, sometimes treated as a separate disease; also: Gerstmann-Sträussler-Scheinker syndrome (GSS) that may be a variant of familial CJD, kuru - probably a result of sporadic CJD's transmission by cannibalism, and fatal familial insomnia (FFI). Their clinical symptoms (and especially of the CJD), are nonspecific and sometimes variable. The imaging, EEG and other laboratory tests are not specific either. Neuropathological studies are needed but their interpretation may be equivocal. TSE's are characterised by the neurodegenerative process with characteristic spongiosis. However, vacuolisation - similar as in TSE-spongiosis - may occur in some CNS's disorders and in the case of putrescent brain tissue. In some cases of CJD, particularly those of long duration, the neuronal loss and astrocyte proliferation can mask the presence of spongiform changes, especially when vacuoles are not numerous. The only certain diagnostic marker for TSE is PrP(Sc), prion protein, presently believed to be a direct cause for all TSEs (TCAs). ThePrP(Sc) has a dominant b-sheet amyloid structure which makes its detection by immunohistochemical procedure possible only with special pretreatment, e.c.: hydrolitic autoclaving, hydrated autoclaving, incubations: formic acid (or guanidine thiocyanate) pretreatment, also combined pretreatments. These methods are standard diagnostic procedures for transmissible cerebral amyloidoses.
 
Lista artykułów w numerze :
Numer: 2
Tytuł: PSYCHIATRIA POLSKA 2/2004
Wydany: 2004-04-01
Lista wszystkich numerów: zobacz »