Alzheimer’s disease: from molecular mechanism to early diagnosis

Malnar, Martina; Košiček, Marko; Hećimović, Silva

Medicina, Vol. 45 No. 3, 2009.

Pregledni rad

Alzheimer’s disease: from molecular mechanism to early diagnosis

Martina Malnar ; Grupa za istraživanje neurodegenerativnih bolesti , Zavod za molekularnu medicinu, Institut “Ruđer Bošković”, Zagreb, Hrvatska
Marko Košiček ; Grupa za istraživanje neurodegenerativnih bolesti , Zavod za molekularnu medicinu, Institut “Ruđer Bošković”, Zagreb, Hrvatska
Silva Hećimović ; Grupa za istraživanje neurodegenerativnih bolesti , Zavod za molekularnu medicinu, Institut “Ruđer Bošković”, Zagreb, Hrvatska

Puni tekst: hrvatski pdf 1.460 Kb

str. 234-243

preuzimanja: 3.894

citiraj

APA 6th Edition

Malnar, M., Košiček, M. i Hećimović, S. (2009). Alzheimer’s disease: from molecular mechanism to early diagnosis. Medicina Fluminensis, 45 (3), 0-0. Preuzeto s https://hrcak.srce.hr/43664

MLA 8th Edition

Malnar, Martina, et al. "Alzheimer’s disease: from molecular mechanism to early diagnosis." Medicina Fluminensis, vol. 45, br. 3, 2009, str. 0-0. https://hrcak.srce.hr/43664. Citirano 20.11.2024.

Chicago 17th Edition

Malnar, Martina, Marko Košiček i Silva Hećimović. "Alzheimer’s disease: from molecular mechanism to early diagnosis." Medicina Fluminensis 45, br. 3 (2009): 0-0. https://hrcak.srce.hr/43664

Harvard

Malnar, M., Košiček, M., i Hećimović, S. (2009). 'Alzheimer’s disease: from molecular mechanism to early diagnosis', Medicina Fluminensis, 45(3), str. 0-0. Preuzeto s: https://hrcak.srce.hr/43664 (Datum pristupa: 20.11.2024.)

Vancouver

Malnar M, Košiček M, Hećimović S. Alzheimer’s disease: from molecular mechanism to early diagnosis. Medicina Fluminensis [Internet]. 2009 [pristupljeno 20.11.2024.];45(3). Dostupno na: https://hrcak.srce.hr/43664

IEEE

M. Malnar, M. Košiček i S. Hećimović, "Alzheimer’s disease: from molecular mechanism to early diagnosis", Medicina Fluminensis, vol.45, br. 3, str. 0-0, 2009. [Online]. Dostupno na: https://hrcak.srce.hr/43664. [Citirano: 20.11.2024.]

Sažetak

Alzheimer’s disease (AD) is the most common form of dementi a. Although the
disease and its main pathological features, senile plaques and neurofi brillary tangles, have
been discovered over 100 years ago, there is sti ll no adequate therapy that would treat,
slow progression or prevent the genesis of Alzheimer’s disease. Since altered metabolism of
the β-amyloid precursor protein (APP) and altered formati on of amyloid-β pepti de (Aβ) play
a central role in the pathogenesis of Alzheimer’s disease, understanding their mechanism of
formati on and clearance is important for designing new therapies for AD. Development of
novel diagnosti c methods that will enable early and accurate diagnosis of AD is of high importance.
It is esti mated that any new interventi on against AD will have its greatest eff ect if
applied early in the pathogenesis of the disease, when the brain is not that much aff ected.
Anaylsis of the three proteins in the cerebrospinal fl uid (CSF) (Aβ42, total tau and phoshotau)
gave the best results unti l now and showed that this test could be used for diff erenti al
diagnosis of AD as well as for diagnosis of non-demented individuals and mildly cogniti vely
impaired (MCI) individuals who will progress to AD in the future. Thus, the goal of the biomarker
research is to identi fy changes that will diagnose AD in its earliest stage. We hope
that diff erent aspects of reserach on AD will generate novel therapies and/or will help in
preventi ng Alzheimer’s disease.

Ključne riječi

amyloid-β; cerebrospinal fluid; dementia; diagnosis; tau

Hrčak ID:

43664

URI

https://hrcak.srce.hr/43664

Datum izdavanja:

1.9.2009.

Podaci na drugim jezicima: hrvatski

Posjeta: 6.238 *

Prijava i registracija

Medicina, Vol. 45 No. 3, 2009.

Sažetak

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