TDP-43 pathology in anterior temporal pole cortex in aging and Alzheimer’s disease

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Abstract

TDP-43 pathology was investigated in the anterior temporal pole cortex (ATPC) and orbital frontal cortex (OFC), regions often degenerated in frontotemporal lobar degenerations (FTLD), in aging and Alzheimer’s disease (AD). Diagnosis of dementia in the 1160 autopsied participants from 3 studies of community-dwelling elders was based on clinical evaluation and cognitive performance tests which were used to create summary measures of the five cognitive domains. Neuronal and glial TDP-43 cytoplasmic inclusions were quantitated in 8 brain regions by immunohistochemistry, and used in ANOVA and regression analyses. TDP-43 pathology was present in 547 (49.4%) participants in whom ATPC (41.9%) was the most frequently involved neocortical region and in 15.5% of these cases, ATPC was the only neocortical area with TDP-43 pathology suggesting not only that ATPC is involved early by TDP-43 but that ATPC may represent an intermediate stage between mesial temporal lobe involvement by TDP-43 and the last stage with involvement of other neocortical areas. To better study this intermediary neocortical stage, and to integrate with other staging schemes, our previous 3 stage distribution of TDP-43 pathology was revised to a 5 stage distribution scheme with stage 1 showing involvement of the amygdala only; stage 2 showed extension to hippocampus and/or entorhinal cortex; stage 3 showed extension to the ATPC; stage 4 – showed extension to the midtemporal cortex and/or OFC and finally in stage 5, there was extension to the midfrontal cortex. Clinically, cases in stages 2 to 5 had impaired episodic memory, however, stage 3 was distinct from stage 2 since stage 3 cases had significantly increased odds of dementia. The proportion of cases with hippocampal sclerosis increased progressively across the stages with stage 5 showing the largest proportion of hippocampal sclerosis cases. Stage 5 cases differed from other stages by having impairment of semantic memory and perceptual speed, in addition to episodic memory impairment. These data suggest that of the regions studied, TDP-43 pathology in the ATPC is an important early neocortical stage of TDP-43 progression in aging and AD while extension of TDP-43 pathology to the midfrontal cortex is a late stage associated with more severe and global cognitive impairment.

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Decision Rules Guiding the Clinical Diagnosis of Alzheimer’s Disease in Two Community-Based Cohort Studies Compared to Standard Practice in a Clinic-Based Cohort Study

David Bennett, Julie Schneider, Neelum Aggarwal … (2006)

We developed prediction rules to guide the clinical diagnosis of Alzheimer’s disease (AD) in two community-based cohort studies (the Religious Orders Study and the Rush Memory and Aging Project). The rules were implemented without informant interviews, neuroimaging, blood work or routine case conferencing. Autopsies were performed at death and the pathologic diagnosis of AD made with a modified version of the Consortium to Establish a Registry for Alzheimer’s Disease (CERAD) criteria. We compared the positive predictive value of the clinical diagnosis in the two community-based studies to the positive predictive value of the clinical diagnosis of AD made by standard clinical practice in a clinic-based cohort study using AD pathology as the gold standard. Of 306 clinic cases with probable AD, 286 (93.5%) met CERAD neuropathologic criteria for AD; the results were comparable for those with possible AD (51 of 54, 94.4%). Of 141 study subjects with probable AD, 130 (92.2%) met CERAD neuropathologic criteria for AD; the results were lower but acceptable for those with possible AD (26 of 37, 70.3%). The results were similar in secondary analyses using alternate neuropathologic criteria for AD. The clinical diagnosis of AD can be made in community-based studies without the use of informant interviews, neuroimaging, blood work or routine case conferencing. This approach holds promise for reducing the operational costs of epidemiologic studies of aging and AD.

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Co-morbidity of TDP-43 proteinopathy in Lewy body related diseases.

Steven E. Arnold, Douglas Galasko, Jessica Lee … (2007)

Here, we investigated if TAR-DNA-binding protein-43 (TDP-43), the disease protein in frontotemporal lobar degeneration and ubiquitin inclusions with or without motor neuron disease as well as amyotrophic lateral sclerosis, also formed inclusions in Lewy body (LB) disorders including Parkinson's disease (PD) without or with dementia (PDD), and dementia with LBs (DLB) alone or in association with Alzheimer's disease (AD). Immunohistochemical analyses of TDP-43 in clinically well characterized and pathologically confirmed cases of DLB + AD, PD and PDD demonstrated TDP-43 pathology in the following percentage of cases: DLB + AD = 25/80 (31.3%); PD = 5/69 (7.2%); PDD = 4/21 (19%), while DLB and normal controls exhibited no (0/10, 0%) and one cases (1/33, 3%) presenting TDP-43 pathology, respectively. Significant differences in the prevalence of TDP-43 lesions were noted between disease versus normal brains (P < 0.001) as well as demented versus non-demented brains (P < 0.001). Statistical analyses revealed a positive relationship between TDP-43 lesions and several clinical and pathological parameters in these disorders suggesting the TDP-43 pathology may have co-morbid effects in LB diseases. This study expands the concept of TDP-43 proteinopathies by implicating TDP-43 lesions in mechanisms of neurodegeneration in LB disorders.

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Hippocampal sclerosis and TDP-43 pathology in aging and Alzheimer disease.

Sukriti Nag, Lei Yu, Ana Capuano … (2015)

To investigate the association of hippocampal sclerosis (HS) with TAR-DNA binding protein of 43kDa (TDP-43) and other common age-related pathologies, dementia, probable Alzheimer disease (AD), mild cognitive impairment (MCI), and cognitive domains in community-dwelling older subjects.

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Author and article information

Contributors

Sukriti Nag: 312-942-2269 , Sukriti_Nag@rush.edu

Lei Yu: Lei_Yu@rush.edu

Patricia A. Boyle: Patricia_Boyle@rush.edu

Sue E. Leurgans: Sue_E_Leurgans@rush.edu

David A. Bennett: David_A_Bennett@rush.edu

Julie A. Schneider: Julie_A_Schneider@rush.edu

Journal

Journal ID (nlm-ta): Acta Neuropathol Commun

Journal ID (iso-abbrev): Acta Neuropathol Commun

Title: Acta Neuropathologica Communications

Publisher: BioMed Central (London )

ISSN (Electronic): 2051-5960

Publication date (Electronic): 1 May 2018

Publication date PMC-release: 1 May 2018

Publication date Collection: 2018

Volume: 6

Electronic Location Identifier: 33

Affiliations

[1 ]ISNI 0000 0001 0705 3621, GRID grid.240684.c, Rush Alzheimer Disease Center, , Rush University Medical Center, ; Suite 1000, 1750 W Harrison Street, Chicago, IL 60612 USA

[2 ]ISNI 0000 0001 0705 3621, GRID grid.240684.c, Departments of Pathology (Neuropathology), , Rush University Medical Center, ; Chicago, IL USA

[3 ]ISNI 0000 0001 0705 3621, GRID grid.240684.c, Departments of Neurological Sciences, , Rush University Medical Center, ; Chicago, IL USA

[4 ]ISNI 0000 0001 0705 3621, GRID grid.240684.c, Departments of Behavioral Sciences, , Rush University Medical Center, ; Chicago, IL USA

Article

Publisher ID: 531

DOI: 10.1186/s40478-018-0531-3

PMC ID: 5928580

PubMed ID: 29298724

SO-VID: 07b19084-7829-49ef-90a1-933751abcb82

License:

Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License ( http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver ( http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.

History

Date received : 4 April 2018

Date accepted : 5 April 2018

Funding

Funded by: FundRef http://dx.doi.org/10.13039/100000049, National Institute on Aging;

Award ID: R01AG017917

Award ID: P30AG010161

Award ID: R01AG042210

Award ID: RF1AG022018

Award Recipient : David A. Bennett Julie A. Schneider

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Keywords: alzheimer’s disease,anterior temporal pole,dementia,episodic memory,hippocampal sclerosis,orbital frontal cortex,semantic memory,tdp-43

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Keywords: alzheimer’s disease, anterior temporal pole, dementia, episodic memory, hippocampal sclerosis, orbital frontal cortex, semantic memory, tdp-43

TDP-43 pathology in anterior temporal pole cortex in aging and Alzheimer’s disease

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Karger: Neurology and Neuroscience

Most cited references 15

Decision Rules Guiding the Clinical Diagnosis of Alzheimer’s Disease in Two Community-Based Cohort Studies Compared to Standard Practice in a Clinic-Based Cohort Study

Co-morbidity of TDP-43 proteinopathy in Lewy body related diseases.

Hippocampal sclerosis and TDP-43 pathology in aging and Alzheimer disease.

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