User: Guest  Login
If you experience problems opening the document, please try this link.
Original title:
Clearance-Mechanismen von Amyloid-β bei der Alzheimer-Krankheit
Translated title:
Clearance mechanisms of β-amyloid in Alzheimer’s disease
Author:
Goldhardt, Oliver
Year:
2019
Document type:
Dissertation
Faculty/School:
Fakultät für Medizin
Advisor:
Grimmer, Timo (Prof. Dr.)
Referee:
Grimmer, Timo (Prof. Dr.); Förstl, Johann (Prof. Dr.)
Language:
de
Subject group:
MED Medizin; PSY Psychologie
Keywords:
Amyloid-β, Alzheimer, Neprilysin, Low-Density-Lipoprotein Receptor-related Protein 1, LRP-1, NEP
Translated keywords:
β-amyloid, Alzheimer, Neprilysin, Low-Density-Lipoprotein Receptor-related Protein 1, LRP-1, NEP
TUM classification:
MED 600d; PSY 750d
Abstract:
Eine gestörte Amyloid(Aβ)-Clearance wird als Ursache der sporadischen Alzheimer-Krankheit vermutet. Zwei Clearance-Mechanismen wurden an Patienten untersucht: Das T-Allel des C667T-Polymorphismus des Low-Density-Lipoprotein Receptor-related Protein 1 (LRP-1)-Transportergens korrelierte mit der zerebralen Aβ-Menge. Die anti-amyloiderge Neprilysin-Aktivität im Liquor (NEP) war positiv mit Biomarkern für neuronale Schädigung korreliert und invers mit der Aβ42-Liquorkonzentration.
Translated abstract:
An impaired amyloid (Aβ) clearance is a suspected cause in sporadic Alzheimer’s disease. Two mechanisms of Aβ clearance have been investigated in patients: The T allele of the C667T polymorphism of the Low-Density-Lipoprotein Receptor-related Protein 1 (LRP-1) transporter gene was positively associated with the cerebral amyloid load. The anti-amyoidogenic NEP activity in the CSF (NEP) was positively associated with biomarkers for neuronal injury and inversely with the CSF-Aβ42 concentration.
WWW:
https://mediatum.ub.tum.de/?id=1507336
Date of submission:
01.07.2019
Oral examination:
20.12.2019
File size:
1142313 bytes
Pages:
58
Urn (citeable URL):
https://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:91-diss-20191220-1507336-1-2
Last change:
24.01.2020
 BibTeX