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Prevalence and Clinical Phenotype of Quadruple Misfolded Proteins in Older Adults
JAMA Neurol. 2020 Oct 1;77(10):1299-1307. doi: 10.1001/jamaneurol.2020.1741.
Shama Karanth 1 2, Peter T Nelson 2 3, Yuriko Katsumata 2 4, Richard J Kryscio 2 4 5, Frederick A Schmitt 2 6, David W Fardo 2 4, Matthew D Cykowski 7, Gregory A Jicha 2 6, Linda J Van Eldik 2 8, Erin L Abner 1 2 4
Abstract:
Importance: Quadruple misfolded proteins (tau neurofibrillary tangles, amyloid-β [Aβ], α-synuclein, and transactive response DNA-binding protein 43 [TDP-43]) in the same brain are relatively common in aging. However, the clinical presentation, associated factors, frequency in community-based cohorts, genetic characteristics, and cognitive trajectories associated with the quadruple misfolded proteins phenotype are not well understood.
Objective: To describe the quadruple misfolded proteins phenotype, including the trajectories of global cognition, in an autopsy cohort.
Design, setting, and participants: This retrospective cohort study used brain autopsy data from the University of Kentucky Alzheimer Disease Center (UK-ADC) Brain Bank. Participants were deceased individuals who were enrolled in a longitudinal community-based cohort study of aging and dementia in central Kentucky conducted by the UK-ADC. Included participants were enrolled in the UK-ADC cohort between January 1, 1989, and December 31, 2017; aged 55 years or older at baseline; and followed up for a mean duration of 10.4 years. The participants had Alzheimer disease pathology (tau and Aβ), α-synuclein, and TDP-43 data, along with Braak neurofibrillary tangle stage I to VI. Data analysis was conducted between February 1, 2019, and September 30, 2019.
Main outcomes and measures: Frequency of quadruple misfolded proteins was estimated, and proteinopathy group characteristics and associations with global cognition were evaluated. Multinomial logistic regression was used to estimate the association of proteinopathy group with participant characteristics, including age at death, sex, and apolipoprotein ε4 (APOE ε4) allele. Generalized estimating equations were used to estimate the probability of obtaining Mini-Mental State Examination (MMSE) scores within the normal cognition (27-30 points) and severe impairment (≤13 points) ranges during the 12 years before death.
Results: The final sample included 375 individuals (mean [SD] age at death, 86.9 [8.0] years); 232 women [61.9%]). Quadruple misfolded proteins were detected in 41 of 214 individuals with dementia (19.2%). Overall, 46 individuals (12.3%) had quadruple misfolded proteins, whereas 143 individuals (38.1%) had 3 proteinopathies. Dementia frequency was highest among those with quadruple misfolded proteins (41 [89.1%]), and participants with quadruple misfolded proteins had the lowest final mean (SD) MMSE scores of 13.4 (9.8) points. Adjusting for age at death and sex, the APOE ε4 allele was associated with higher odds of quadruple misfolded proteins (adjusted odds ratio, 2.55; 95% CI, 1.16- 5.62; P = .02). The quadruple misfolded proteins group had both the lowest probability of obtaining MMSE scores in the normal cognition range, even 12 years before death, and the highest probability of having MMSE scores in the severe impairment range.
Conclusions and relevance: Quadruple misfolded proteins appear to be a common substrate for cognitive impairment and to be associated with an aggressive course of disease that typically ends with severe dementia. The prevalence of comorbid α-synuclein and TDP-43 with Alzheimer disease pathology (tau and Aβ) may complicate efforts to identify therapies to treat and prevent Alzheimer disease.
Conflict of interest statementConflict of Interest Disclosures: Dr Schmitt reported receiving grants from the National Institute on Aging (NIA) and the Eunice Kennedy Shriver National Institute of Child Health and Human Development during the conduct of the study. Dr Fardo reported receiving grants from the NIA, the National Institute on Drug Abuse, and the National Heart, Lung, and Blood Institute. Dr Jicha reported receiving grants from the National Institute of Health during the conduct of the study and grants from Alltech, Biohaven, Eisai, Lilly, Novartis, and Suven outside the submitted work. Dr Van Eldik reported receiving grants from the NIA National Institute of Neurological Disorders and Stroke, and the Alzheimer Drug Discovery Foundation during the conduct of the study. Dr. Kryscio reported receiving support from the NIA, the National Institute on Neurological Diseases and Stroke, and the National Center for Translational Sciences. Dr Abner reported receiving grants from the NIA during the conduct of the study. No other disclosures were reported.
Objective: To describe the quadruple misfolded proteins phenotype, including the trajectories of global cognition, in an autopsy cohort.
Design, setting, and participants: This retrospective cohort study used brain autopsy data from the University of Kentucky Alzheimer Disease Center (UK-ADC) Brain Bank. Participants were deceased individuals who were enrolled in a longitudinal community-based cohort study of aging and dementia in central Kentucky conducted by the UK-ADC. Included participants were enrolled in the UK-ADC cohort between January 1, 1989, and December 31, 2017; aged 55 years or older at baseline; and followed up for a mean duration of 10.4 years. The participants had Alzheimer disease pathology (tau and Aβ), α-synuclein, and TDP-43 data, along with Braak neurofibrillary tangle stage I to VI. Data analysis was conducted between February 1, 2019, and September 30, 2019.
Main outcomes and measures: Frequency of quadruple misfolded proteins was estimated, and proteinopathy group characteristics and associations with global cognition were evaluated. Multinomial logistic regression was used to estimate the association of proteinopathy group with participant characteristics, including age at death, sex, and apolipoprotein ε4 (APOE ε4) allele. Generalized estimating equations were used to estimate the probability of obtaining Mini-Mental State Examination (MMSE) scores within the normal cognition (27-30 points) and severe impairment (≤13 points) ranges during the 12 years before death.
Results: The final sample included 375 individuals (mean [SD] age at death, 86.9 [8.0] years); 232 women [61.9%]). Quadruple misfolded proteins were detected in 41 of 214 individuals with dementia (19.2%). Overall, 46 individuals (12.3%) had quadruple misfolded proteins, whereas 143 individuals (38.1%) had 3 proteinopathies. Dementia frequency was highest among those with quadruple misfolded proteins (41 [89.1%]), and participants with quadruple misfolded proteins had the lowest final mean (SD) MMSE scores of 13.4 (9.8) points. Adjusting for age at death and sex, the APOE ε4 allele was associated with higher odds of quadruple misfolded proteins (adjusted odds ratio, 2.55; 95% CI, 1.16- 5.62; P = .02). The quadruple misfolded proteins group had both the lowest probability of obtaining MMSE scores in the normal cognition range, even 12 years before death, and the highest probability of having MMSE scores in the severe impairment range.
Conclusions and relevance: Quadruple misfolded proteins appear to be a common substrate for cognitive impairment and to be associated with an aggressive course of disease that typically ends with severe dementia. The prevalence of comorbid α-synuclein and TDP-43 with Alzheimer disease pathology (tau and Aβ) may complicate efforts to identify therapies to treat and prevent Alzheimer disease.
Conflict of interest statementConflict of Interest Disclosures: Dr Schmitt reported receiving grants from the National Institute on Aging (NIA) and the Eunice Kennedy Shriver National Institute of Child Health and Human Development during the conduct of the study. Dr Fardo reported receiving grants from the NIA, the National Institute on Drug Abuse, and the National Heart, Lung, and Blood Institute. Dr Jicha reported receiving grants from the National Institute of Health during the conduct of the study and grants from Alltech, Biohaven, Eisai, Lilly, Novartis, and Suven outside the submitted work. Dr Van Eldik reported receiving grants from the NIA National Institute of Neurological Disorders and Stroke, and the Alzheimer Drug Discovery Foundation during the conduct of the study. Dr. Kryscio reported receiving support from the NIA, the National Institute on Neurological Diseases and Stroke, and the National Center for Translational Sciences. Dr Abner reported receiving grants from the NIA during the conduct of the study. No other disclosures were reported.
PMID: 32568358
Free Full-Text: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7309572/