% IMPORTANT: The following is UTF-8 encoded. This means that in the presence
% of non-ASCII characters, it will not work with BibTeX 0.99 or older.
% Instead, you should use an up-to-date BibTeX implementation like “bibtex8” or
% “biber”.
@ARTICLE{Richter:1050016,
author = {Richter, Nils and Onur, Oezguer A. and Fink, Gereon R.},
title = {{D}etecting limbic predominant neurodegenerative
co-pathologies in vivo in {A}lzheimer’s disease: magnetic
resonance imaging markers, cognitive correlates, and
prognosis},
journal = {Alzheimer's research $\&$ therapy},
volume = {17},
number = {1},
issn = {1758-9193},
address = {London},
publisher = {BioMed Central},
reportid = {FZJ-2025-05730},
pages = {236},
year = {2025},
note = {Open Access funding enabled and organized by Projekt DEAL.
Datacollection and sharing for this project was funded by
the Alzheimer'sDisease Neuroimaging Initiative (ADNI)
(National Institutes of Health GrantU01 AG024904) and DOD
ADNI (Department of Defense award numberW81XWH-12-2-0012).
ADNI is funded by the National Institute on Aging,
theNational Institute of Biomedical Imaging and
Bioengineering, and throughgenerous contributions from the
following: AbbVie, Alzheimer’s Association;Alzheimer’s
Drug Discovery Foundation; Araclon Biotech; BioClinica,
Inc.;Biogen; Bristol-Myers Squibb Company; CereSpir, Inc.;
Cogstate; Eisai Inc.;Elan Pharmaceuticals, Inc.; Eli Lilly
and Company; EuroImmun; F. Hoffmann-LaRoche Ltd and its
affiliated company Genentech, Inc.; Fujirebio; GE
Healthcare;IXICO Ltd.; Janssen Alzheimer Immunotherapy
Research $\&$ Development,LLC.; Johnson $\&$ Johnson
Pharmaceutical Research $\&$ Development LLC.;Lumosity;
Lundbeck; Merck $\&$ Co., Inc.; Meso Scale Diagnostics,
LLC.; NeuroRxResearch; Neurotrack Technologies; Novartis
Pharmaceuticals Corporation;Pfizer Inc.; Piramal Imaging;
Servier; Takeda Pharmaceutical Company;and Transition
Therapeutics. The Canadian Institutes of Health Researchis
providing funds to support ADNI clinical sites in Canada.
Private sectorcontributions are facilitated by the
Foundation for the National Institutes ofHealth
(www.fnih.org). The grantee organization is the Northern
CaliforniaInstitute for Research and Education, and the
study is coordinated by theAlzheimer’s Therapeutic
Research Institute at the University of SouthernCalifornia.
ADNI data are disseminated by the Laboratory for Neuro
Imagingat the University of Southern California.This work
was supported by agrant from the Marga and Walter Boll
Foundation (Nr. 210–08-13), Kerpen,Germany, to GRF and
OO.Open access publication funded by the
DeutscheForschungsgemeinschaft (DFG, German Research
Foundation) – 491111487.},
abstract = {In Alzheimer's disease (AD), limbic non-AD co-pathologies
are common and contribute to memory impairment and
accelerated clinical progression. To date, in vivo
biomarkers of these co-pathologies are lacking. Here, we
examined whether specific regional gray matter (GM) atrophy
patterns on magnetic resonance imaging (MRI) allow
distinguishing between patients with 'pure' AD pathology and
those with AD pathology and limbic non-AD co-pathologies
(AD+).Methods: Atrophy patterns based on ante-mortem MRI
scans of histopathologically confirmed 'pure' AD (n = 36)
and AD+, i.e., AD pathology with concomitant limbic TDP-43
pathology and argyrophilic grain disease (n = 39), were
applied to classify an independent cohort of clinically
diagnosed patients with mild cognitive impairment (MCI, n =
224) and dementia (n = 221). Furthermore, we examined the
degree to which an MRI marker of cortical degeneration
reflecting tau pathology could improve the estimation of
clinical progression.Results: Histopathologically confirmed
AD+ pathology was associated with more substantial
hippocampal atrophy but less cortical degeneration in
intermediate Braak stage regions than 'pure' AD pathology.
Clinically diagnosed AD patients with an AD+-classified
ratio of cortical-to-hippocampal GM exhibited significantly
more memory impairment. At the stage of MCI, AD+-classified
atrophy was also associated with speeded clinical decline.
Furthermore, tau-associated cortical degeneration emerged as
the primary predictor of clinical progression across groups
and disease stages.Conclusions: The data suggest that in MCI
due to AD, additional non-AD limbic co-pathologies are
associated with greater hippocampal but less cortical
atrophy and more rapid clinical decline. In contrast, in
mild dementia due to AD, hippocampal GM was not associated
with prognosis. Instead, cortical degeneration appeared to
drive clinical progression.Keywords: Argyrophilic grain
disease; Braak stages; Dementia; Limbic predominant
age-related TDP-43 encephalopathy (LATE); Mild cognitive
impairment; Tau-protein; Voxel-based morphometry.},
cin = {INM-3},
ddc = {610},
cid = {I:(DE-Juel1)INM-3-20090406},
pnm = {5251 - Multilevel Brain Organization and Variability
(POF4-525) / DFG project G:(GEPRIS)491111487 -
Open-Access-Publikationskosten / 2025 - 2027 /
Forschungszentrum Jülich (OAPKFZJ) (491111487)},
pid = {G:(DE-HGF)POF4-5251 / G:(GEPRIS)491111487},
typ = {PUB:(DE-HGF)16},
doi = {10.1186/s13195-025-01885-6},
url = {https://juser.fz-juelich.de/record/1050016},
}
Gast ::