Creutzfeldt-Jakob disease: Blood infectivity and screening tests

2001 ◽  
Vol 38 (4, Suppl 9) ◽  
pp. 2-6 ◽  
Author(s):  
Paul Brown
2017 ◽  
Vol 41 (S1) ◽  
pp. S162-S162
Author(s):  
N. De Uribe-viloria ◽  
M. De Lera Alfonso ◽  
L. Rodriguez Fernandez ◽  
G. Zapico Aldea ◽  
C. Laserna Del Gallego ◽  
...  

IntroductionNeurocognitive disorders are the only psychiatric disorders which underlying pathogeny can potentially be determined. This has important implications, for it makes possible the use of biomarkers in order to gain better diagnosis, and opens a door to more accurate treatments. Nonetheless, as biomarkers are not exclusive of a single disorder, the lengths of its utility are still unknown.Objectives and aimsTo understand the values and limitations of biomarkers in differential diagnosis of dementias.MethodsWe present three cases followed in the Neurology ward of our hospital, in which they were admitted for diagnosis and treatment of a subacute form of dementia. Medical history, core symptoms, screening tests for cognitive impairment, MRI, EEG and biomarkers in cerebrospinal fluid were used for diagnosis.ResultsTwo cases had consistent clinical features and complementary explorations, and they were respectively diagnosed as Creutzfeldt-Jakob Disease and Lewy Body Dementia; however, the last case showed contradictory results between clinic and complementary explorations, particularly 14-3-3 protein, which was positive and led to the initial diagnosis as Creutzfeldt-Jakob Disease, which was proven wrong once necropsy was practiced.ConclusionsAlthough complementary explorations, and biomarkers in particular, are of invaluable utility in the accurate diagnosis of multiple psychiatric diseases, they must always be considered within a context given by biography and clinical features, because, when failing to do so, they can lead to misdiagnosis and delay of correct treatment.


Author(s):  
F. G. Zaki ◽  
E. Detzi ◽  
C. H. Keysser

This study represents the first in a series of investigations carried out to elucidate the mechanism(s) of early hepatocellular damage induced by drugs and other related compounds. During screening tests of CNS-active compounds in rats, it has been found that daily oral administration of one of these compounds at a dose level of 40 mg. per kg. of body weight induced diffuse massive hepatic necrosis within 7 weeks in Charles River Sprague Dawley rats of both sexes. Partial hepatectomy enhanced the development of this peculiar type of necrosis (3 weeks instead of 7) while treatment with phenobarbital prior to the administration of the drug delayed the appearance of necrosis but did not reduce its severity.Electron microscopic studies revealed that early development of this liver injury (2 days after the administration of the drug) appeared in the form of small dark osmiophilic vesicles located around the bile canaliculi of all hepatocytes (Fig. 1). These structures differed from the regular microbodies or the pericanalicular multivesicular bodies. They first appeared regularly rounded with electron dense matrix bound with a single membrane. After one week on the drug, these vesicles appeared vacuolated and resembled autophagosomes which soon developed whorls of concentric lamellae or cisterns characteristic of lysosomes (Fig. 2). These lysosomes were found, later on, scattered all over the hepatocytes.


2015 ◽  
Vol 72 (4) ◽  
pp. 219-224 ◽  
Author(s):  
Stephanie A. Bridenbaugh

Es gibt eine starke Assoziation zwischen Kognition und Mobilität. Ältere Erwachsene mit Gangdefiziten haben ein erhöhtes Risiko, kognitive Defizite, sogar eine Demenz, zu entwickeln. Kognitive Defizite wiederum sind mit einer Verschlechterung des Gehens assoziiert. Sowohl kognitive als auch Mobilitätsdefizite sind mit einem erhöhten Sturzrisiko verbunden. Untersuchungen der Kognition, vor allem der Exekutivfunktionen, und die funktionale Mobilität sollen daher ein wesentlicher Bestandteil jedes umfassenden geriatrischen Assessments sein. Einige schnelle Screening-Tests können in der Hausarztpraxis durchgeführt werden, um Mobilitätsprobleme zu erfassen. Falls diese pathologisch ausfallen, sollten genauere Ganguntersuchungen veranlasst werden. Bei Untersuchungen des Ganges sind Dual-Task Paradigmen (Gehen und gleichzeitig eine andere Aufgaben ausführen) besonders aussagekräftig in der Früherkennung von Mobilitäts- und auch Hirnleistungsdefiziten. Die Früherkennung erlaubt eine frühzeitige Implementierung von gezielten Interventionen, um die Gangsicherheit und möglicherweise auch gewisse Hirnleistungen zu verbessern.


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