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January 10, 2023; 100 (2) Research Article

Impact and Risk Factors of Limbic Predominant Age-Related TDP-43 Encephalopathy Neuropathologic Change in an Oldest-Old Cohort

View ORCID ProfileSeyed Ahmad Sajjadi, Syed Bukhari, Kiana A. Scambray, Rui Yan, Claudia Kawas, Thomas J. Montine, Maria M. Corrada
First published October 27, 2022, DOI: https://doi.org/10.1212/WNL.0000000000201345
Seyed Ahmad Sajjadi
From the University of California (S.A.S., K.A.S., R.Y., C.K., M.M.C.), Irvine; and Stanford University (S.B., T.J.M.), CA.
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  • ORCID record for Seyed Ahmad Sajjadi
Syed Bukhari
From the University of California (S.A.S., K.A.S., R.Y., C.K., M.M.C.), Irvine; and Stanford University (S.B., T.J.M.), CA.
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Kiana A. Scambray
From the University of California (S.A.S., K.A.S., R.Y., C.K., M.M.C.), Irvine; and Stanford University (S.B., T.J.M.), CA.
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Rui Yan
From the University of California (S.A.S., K.A.S., R.Y., C.K., M.M.C.), Irvine; and Stanford University (S.B., T.J.M.), CA.
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Claudia Kawas
From the University of California (S.A.S., K.A.S., R.Y., C.K., M.M.C.), Irvine; and Stanford University (S.B., T.J.M.), CA.
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Thomas J. Montine
From the University of California (S.A.S., K.A.S., R.Y., C.K., M.M.C.), Irvine; and Stanford University (S.B., T.J.M.), CA.
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Maria M. Corrada
From the University of California (S.A.S., K.A.S., R.Y., C.K., M.M.C.), Irvine; and Stanford University (S.B., T.J.M.), CA.
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Impact and Risk Factors of Limbic Predominant Age-Related TDP-43 Encephalopathy Neuropathologic Change in an Oldest-Old Cohort
Seyed Ahmad Sajjadi, Syed Bukhari, Kiana A. Scambray, Rui Yan, Claudia Kawas, Thomas J. Montine, Maria M. Corrada
Neurology Jan 2023, 100 (2) e203-e210; DOI: 10.1212/WNL.0000000000201345

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Abstract

Background and Objectives Limbic predominant age-related TAR DNA binding protein 43 (TDP-43) encephalopathy neuropathologic change (LATE-NC) is a prevalent degenerative pathology in the oldest-old who are the fastest-growing segment of our population with the highest rates of dementia. We aimed to determine the relationship between LATE-NC and cognitive impairment and to identify its potential risk factors by studying its relationship with common past medical histories in an oldest-old cohort.

Methods Participants from The 90+ Study with longitudinal evaluations and autopsy data were included. Dementia status and impairment in 5 main cognitive domains were determined at postmortem conferences leveraging all clinical and neuropsychological data blind to neuropathologic diagnosis. Medical history information was obtained from patients and their informants. LATE-NC and Alzheimer disease neuropathologic change (ADNC) were considered present in those with TDP-43 pathology in the hippocampus and/or neocortex and those with high likelihood of ADNC according to NIA-AA guidelines, respectively. We examined the association of degenerative pathologies with cognitive outcomes and multiple comparisons–adjusted relationship of medical history variables with LATE-NC and ADNC using logistic regressions adjusted for age at death, sex, and education.

Results Three hundred twenty-eight participants were included in this study. LATE-NC was present in 32% of the participants. It had a significant association with the presence of dementia (OR 2.8, 95% CI 1.7–4.6) and impairment in memory (OR 3.0, 95% CI 1.8–5.1), language (OR 2.6, 95% CI 1.6–4.3), and orientation (OR 3.5, 95% CI 2.1–5.9). The association with impaired orientation was unique to LATE-NC, and the strength and significance of the other associations were comparable to ADNC. Furthermore, we found that history of osteoarthritis (OR 0.37, adjusted 95% CI 0.21–0.66) and hypertension (OR 0.52, adjusted 95% CI 0.28–0.98) were associated with a reduced likelihood of LATE-NC, but not ADNC.

Discussion Our results suggest that LATE-NC is a prevalent degenerative pathology in the oldest-old and has significant associations with dementia and impairment in cognitive domains with magnitudes that are comparable to ADNC. We also found that past medical histories of hypertension and osteoarthritis were associated with a lower likelihood of LATE-NC. This might help identify upstream mechanisms leading to this important pathology.

Glossary

ADNC=
Alzheimer disease neuropathologic change;
CAA=
cerebral amyloid angiopathy;
FTD=
frontotemporal dementia;
HS=
hippocampal sclerosis of aging;
LATE=
limbic predominant age-related TDP-43 encephalopathy;
LATE-NC=
LATE neuropathologic change;
LWCS=
Leisure World Cohort Study;
MMSE=
Mini Mental State Examination;
MVL=
microvascular lesion;
TDP-43=
TAR DNA binding protein 43;
UC=
University of California

Footnotes

  • Go to Neurology.org/N for full disclosures. Funding information and disclosures deemed relevant by the authors, if any, are provided at the end of the article.

  • Submitted and externally peer reviewed. The handling editor was Linda Hershey, MD, PhD, FAAN.

  • Editorial, page 57

  • CME Course: NPub.org/cmelist

  • Received November 8, 2021.
  • Accepted in final form August 19, 2022.
  • © 2022 American Academy of Neurology
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