Your search keyword '"John Q. Trojanowski"' showing total 1,247 results

1. Pathological combinations in neurodegenerative disease are heterogeneous and disease-associated

Author

John L Robinson, Sharon X Xie, Daniel R Baer, EunRan Suh, Vivianna M Van Deerlin, Nicholas J Loh, David J Irwin, Corey T McMillan, David A Wolk, Alice Chen-Plotkin, Daniel Weintraub, Theresa Schuck, Virginia M Y Lee, John Q Trojanowski, and Edward B Lee

Subjects

Neurology (clinical)

Abstract

Pathologies that are causative for neurodegenerative disease (ND) are also frequently present in unimpaired, older individuals. In this retrospective study of 1647 autopsied individuals, we report the incidence of 10 pathologies across ND and normal ageing in attempt to clarify which pathological combinations are disease-associated and which are ageing-related. Eight clinically defined groups were examined including unimpaired individuals and those with clinical Alzheimer’s disease, mixed dementia, amyotrophic lateral sclerosis, frontotemporal degeneration, multiple system atrophy, probable Lewy body disease or probable tauopathies. Up to seven pathologies were observed concurrently resulting in a heterogeneous mix of 161 pathological combinations. The presence of multiple additive pathologies associated with older age, increasing disease duration, APOE e4 allele and presence of dementia across the clinical groups. Fifteen to 67 combinations occurred in each group, with the unimpaired group defined by 35 combinations. Most combinations occurred at a

Published

2023

2. Post-translational modifications of soluble α-synuclein regulate the amplification of pathological α-synuclein

Author

Shujing Zhang, Ruowei Zhu, Buyan Pan, Hong Xu, Modupe F. Olufemi, Ronald J. Gathagan, Yuanxi Li, Luyan Zhang, Jasmine Zhang, Wenxuan Xiang, Eliot Masahiro Kagan, Xingjun Cao, Chaoxing Yuan, Soo-Jung Kim, Christopher K. Williams, Shino Magaki, Harry V. Vinters, Hilal A. Lashuel, Benjamin A. Garcia, E. James Petersson, John Q. Trojanowski, Virginia M.-Y. Lee, and Chao Peng

Subjects

Chromatography, Liquid, Parkinson's Disease, Neurology & Neurosurgery, Synucleinopathies, General Neuroscience, Post-Translational, Neurosciences, Parkinson Disease, Neurodegenerative Diseases, Neurodegenerative, Brain Disorders, Tandem Mass Spectrometry, Neurological, alpha-Synuclein, Acquired Cognitive Impairment, Humans, 2.1 Biological and endogenous factors, Psychology, Cognitive Sciences, Aetiology, Protein Processing

Abstract

Cell-to-cell transmission and subsequent amplification of pathological proteins promote neurodegenerative disease progression. Most research on this has focused on pathological protein seeds, but how their normal counterparts, which are converted to pathological forms during transmission, regulate transmission is less understood. Here we show in cultured cells that phosphorylation of soluble, nonpathological α-synuclein (α-Syn) at previously identified sites dramatically affects the amplification of pathological α-Syn, which underlies Parkinson's disease and other α-synucleinopathies, in a conformation- and phosphorylation site-specific manner. We performed LC-MS/MS analyses on soluble α-Syn purified from Parkinson's disease and other α-synucleinopathies, identifying many new α-Syn post-translational modifications (PTMs). In addition to phosphorylation, acetylation of soluble α-Syn also modified pathological α-Syn transmission in a site- and conformation-specific manner. Moreover, phosphorylation of soluble α-Syn could modulate the seeding properties of pathological α-Syn. Our study represents the first systematic analysis how of soluble α-Syn PTMs affect the spreading and amplification of pathological α-Syn, which may affect disease progression.

Published

2023

3. Cerebrospinal fluid biomarker panel of synaptic dysfunction in Alzheimer's disease and other neurodegenerative disorders

Author

Johanna, Nilsson, Katheryn A Q, Cousins, Johan, Gobom, Erik, Portelius, Alice, Chen-Plotkin, Leslie M, Shaw, Murray, Grossman, David J, Irwin, John Q, Trojanowski, Henrik, Zetterberg, Kaj, Blennow, and Ann, Brinkmalm

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Neurology (clinical), Geriatrics and Gerontology

Abstract

Synaptic degeneration is a key part of the pathophysiology of neurodegenerative diseases, and biomarkers reflecting the pathological alterations are greatly needed.Seventeen synaptic proteins were quantified in a pathology-confirmed cerebrospinal fluid cohort of patients with Alzheimer's disease (AD; n = 63), frontotemporal lobar degeneration (FTLD; n = 53), and Lewy body spectrum of disorders (LBD; n = 21), as well as healthy controls (HC; n = 48).Comparisons revealed four distinct patterns: markers decreased across all neurodegenerative conditions compared to HC (the neuronal pentraxins), markers increased across all neurodegenerative conditions (14-3-3 zeta/delta), markers selectively increased in AD compared to other neurodegenerative conditions (neurogranin and beta-synuclein), and markers selectively decreased in LBD and FTLD compared to HC and AD (AP2B1 and syntaxin-1B).Several of the synaptic proteins may serve as biomarkers for synaptic dysfunction in AD, LBD, and FTLD. Additionally, differential patterns of synaptic protein alterations seem to be present across neurodegenerative diseases.A panel of synaptic proteins were quantified in the cerebrospinal fluid using mass spectrometry. We compared Alzheimer's disease, frontotemporal degeneration, and Lewy body spectrum of disorders. Pathology was confirmed by autopsy or familial mutations. We discovered synaptic biomarkers for synaptic degeneration and cognitive decline. We found differential patterns of synaptic proteins across neurodegenerative diseases.

Published

2022

4. TREM2 risk variants are associated with atypical Alzheimer’s disease

Author

Boram Kim, EunRan Suh, Aivi T. Nguyen, Stefan Prokop, Bailey Mikytuck, Olamide A. Olatunji, John L. Robinson, Murray Grossman, Jeffrey S. Phillips, David J. Irwin, Dawn Mechanic-Hamilton, David A. Wolk, John Q. Trojanowski, Corey T. McMillan, Vivianna M. Van Deerlin, and Edward B. Lee

Subjects

Cellular and Molecular Neuroscience, Membrane Glycoproteins, Alzheimer Disease, Humans, Neurodegenerative Diseases, Neurofibrillary Tangles, Microglia, Neurology (clinical), Receptors, Immunologic, Hippocampus, Pathology and Forensic Medicine

Abstract

Alzheimer's disease (AD) has multiple clinically and pathologically defined subtypes where the underlying causes of such heterogeneity are not well established. Rare TREM2 variants confer significantly increased risk for clinical AD in addition to other neurodegenerative disease clinical phenotypes. Whether TREM2 variants are associated with atypical clinical or pathologically defined subtypes of AD is not known. We studied here the clinical and pathological features associated with TREM2 risk variants in an autopsy-confirmed cohort. TREM2 variant cases were more frequently associated with non-amnestic clinical syndromes. Pathologically, TREM2 variant cases were associated with an atypical distribution of neurofibrillary tangle density with significantly lower hippocampal NFT burden relative to neocortical NFT accumulation. In addition, NFT density but not amyloid burden was associated with an increase of dystrophic microglia. TREM2 variant cases were not associated with an increased prevalence, extent, or severity of co-pathologies. These clinicopathological features suggest that TREM2 variants contribute to clinical and pathologic AD heterogeneity by altering the distribution of neurofibrillary degeneration and tau-dependent microglial dystrophy, resulting in hippocampal-sparing and non-amnestic AD phenotypes.

Published

2022

5. Differential Vulnerability of Hippocampal Subfields in Primary Age-Related Tauopathy and Chronic Traumatic Encephalopathy

Author

Kurt Farrell, Megan A Iida, Jonathan D Cherry, Alicia Casella, Thor D Stein, Kevin F Bieniek, Jamie M Walker, Timothy E Richardson, Charles L White, Victor E Alvarez, Bertrand R Huber, Dennis W Dickson, Ricardo Insausti, Kristen Dams-O'Connor, Jean-Paul Vonsattel, Andy F Teich, Marla Gearing, Jonathan Glass, Juan C Troncoso, Matthew P Frosch, Bradley T Hyman, Melissa E Murray, Johannes Attems, Margaret E Flanagan, Qinwen Mao, M-Marsel Mesulam, Sandra Weintraub, Randy L Woltjer, Thao Pham, Julia Kofler, Julie A Schneider, Lei Yu, Dushyant P Purohit, Vahram Haroutunian, Patrick R Hof, Sam Gandy, Mary Sano, Thomas G Beach, Wayne Poon, Claudia H Kawas, María M Corrada, Robert A Rissman, Jeff Metcalf, Sara Shuldberg, Bahar Salehi, Peter T Nelson, John Q Trojanowski, Edward B Lee, David A Wolk, Corey T McMillan, C Dirk Keene, Caitlin S Latimer, Thomas J Montine, Gabor G Kovacs, Mirjam I Lutz, Peter Fischer, Richard J Perrin, Nigel J Cairns, Ann C McKee, and John F Crary

Subjects

Cellular and Molecular Neuroscience, Neurology, Tauopathies, Humans, Neurofibrillary Tangles, tau Proteins, Neurology (clinical), General Medicine, Hippocampus, Pathology and Forensic Medicine, Chronic Traumatic Encephalopathy

Abstract

Chronic traumatic encephalopathy (CTE) is a tauopathy associated with repetitive mild head impacts characterized by perivascular hyperphosphorylated tau (p-tau) in neurofibrillary tangles (NFTs) and neurites in the depths of the neocortical sulci. In moderate to advanced CTE, NFTs accumulate in the hippocampus, potentially overlapping neuroanatomically with primary age-related tauopathy (PART), an age-related tauopathy characterized by Alzheimer disease-like tau pathology in the hippocampus devoid of amyloid plaques. We measured p-tau burden using positive-pixel counts on immunohistochemically stained and neuroanatomically segmented hippocampal tissue. Subjects with CTE had a higher total p-tau burden than PART subjects in all sectors (p = 0.005). Within groups, PART had significantly higher total p-tau burden in CA1/subiculum compared to CA3 (p = 0.02) and CA4 (p = 0.01) and total p-tau burden in CA2 trended higher than CA4 (p = 0.06). In CTE, total p-tau burden in CA1/subiculum was significantly higher than in the dentate gyrus; and CA2 also trended higher than dentate gyrus (p = 0.01, p = 0.06). When controlling for p-tau burden across the entire hippocampus, CA3 and CA4 had significantly higher p-tau burden in CTE than PART (p lt; 0.0001). These data demonstrate differences in hippocampal p-tau burden and regional distribution in CTE compared to PART that might be helpful in differential diagnosis and reveal insights into disease pathogenesis.

Published

2023

6. Genetic prediction of impulse control disorders in Parkinson's disease

Author

Daniel, Weintraub, Marijan, Posavi, Pierre, Fontanillas, Thomas F, Tropea, Eugenia, Mamikonyan, Eunran, Suh, John Q, Trojanowski, Paul, Cannon, Vivianna M, Van Deerlin, and Alice S, Chen-Plotkin

Subjects

Cohort Studies, Disruptive, Impulse Control, and Conduct Disorders, Logistic Models, General Neuroscience, Humans, Parkinson Disease, Neurology (clinical), Biomarkers

Abstract

To develop a clinico-genetic predictor of impulse control disorder (ICD) risk in Parkinson's disease (PD).In 5770 individuals from three PD cohorts (the 23andMe, Inc.; the University of Pennsylvania [UPenn]; and the Parkinson's Progression Markers Initiative [PPMI]), we used a discovery-replication strategy to develop a clinico-genetic predictor for ICD risk. We first performed a Genomewide Association Study (GWAS) for ICDs anytime during PD in 5262 PD individuals from the 23andMe cohort. We then combined newly discovered ICD risk loci with 13 ICD risk loci previously reported in the literature to develop a model predicting ICD in a Training dataset (n = 339, from UPenn and PPMI cohorts). The model was tested in a non-overlapping Test dataset (n = 169, from UPenn and PPMI cohorts) and used to derive a continuous measure, the ICD-risk score (ICD-RS), enriching for PD individuals with ICD (ICD+ PD).By GWAS, we discovered four new loci associated with ICD at p-values of 4.9e-07 to 1.3e-06In this multi-cohort, international study, we developed an easily computed clinico-genetic tool, the ICD-RS, that substantially enriches for subgroups of PD at very high versus very low risk for ICD, enabling pharmacogenetic approaches to PD medication selection.

Published

2022

7. Glucocerebrosidase activity and lipid levels are related to protein pathologies in Parkinson’s disease

Author

Cheryl E. G. Leyns, Alice Prigent, Brenna Beezhold, Lihang Yao, Nathan G. Hatcher, Peining Tao, John Kang, EunRan Suh, Vivianna M. Van Deerlin, John Q. Trojanowski, Virginia M. Y. Lee, Matthew E. Kennedy, Matthew J. Fell, and Michael X. Henderson

Subjects

Cellular and Molecular Neuroscience, Neurology, Neurology (clinical)

Abstract

Parkinson’s disease (PD) and dementia with Lewy bodies (DLB) are progressive neurodegenerative diseases characterized by the accumulation of misfolded α-synuclein in the form of Lewy pathology. While most cases are sporadic, there are rare genetic mutations that cause disease and more common variants that increase incidence of disease. The most prominent genetic mutations for PD and DLB are in the GBA1 and LRRK2 genes. GBA1 mutations are associated with decreased glucocerebrosidase activity and lysosomal accumulation of its lipid substrates, glucosylceramide and glucosylsphingosine. Previous studies have shown a link between this enzyme and lipids even in sporadic PD. However, it is unclear how the protein pathologies of disease are related to enzyme activity and glycosphingolipid levels. To address this gap in knowledge, we examined quantitative protein pathology, glucocerebrosidase activity and lipid substrates in parallel from 4 regions of 91 brains with no neurological disease, idiopathic, GBA1-linked, or LRRK2-linked PD and DLB. We find that several biomarkers are altered with respect to mutation and progression to dementia. We found mild association of glucocerebrosidase activity with disease, but a strong association of glucosylsphingosine with α-synuclein pathology, irrespective of genetic mutation. This association suggests that Lewy pathology precipitates changes in lipid levels related to progression to dementia.

Published

2023

8. Preclinical characterization and IND‐enabling safety studies for PNT001, an antibody that recognizes cis ‐pT231 tau

Author

Kelly Foster, Matteo Manca, Kim McClure, Pyry Koivula, John Q. Trojanowski, Daniel Havas, Sarah Chancellor, Lee Goldstein, Kurt R. Brunden, Allison Kraus, and Michael K. Ahlijanian

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Neurology (clinical), Geriatrics and Gerontology

Published

2023

9. Divergent Histopathological Networks of Frontotemporal Degeneration Proteinopathy Subytpes

Author

Min Chen, Daniel T. Ohm, Jeffrey S. Phillips, Corey T. McMillan, Noah Capp, Claire Peterson, Emily Xie, David A. Wolk, John Q. Trojanowski, Edward B. Lee, James Gee, Murray Grossman, and David J. Irwin

Subjects

Tauopathies, Frontotemporal Dementia, TDP-43 Proteinopathies, General Neuroscience, Disease Progression, Humans, tau Proteins, Atrophy, Frontotemporal Lobar Degeneration

Abstract

Network analyses inform complex systems such as human brain connectivity, but this approach is seldom applied to gold-standard histopathology. Here, we use two complimentary computational approaches to model microscopic progression of the main subtypes of tauopathy versus TDP-43 proteinopathy in the human brain. Digital histopathology measures were obtained in up to 13 gray matter (GM) and adjacent white matter (WM) cortical brain regions sampled from 53 tauopathy and 66 TDP-43 proteinopathy autopsy patients. First, we constructed a weighted non-directed graph for each group, where nodes are defined as GM and WM regions sampled and edges in the graph are weighted using the group-level Pearson's correlation coefficient for each pairwise node comparison. Additionally, we performed mediation analyses to test mediation effects of WM pathology between anterior frontotemporal and posterior parietal GM nodes. We find greater correlation (i.e., edges) between GM and WM node pairs in tauopathies compared with TDP-43 proteinopathies. Moreover, WM pathology strongly correlated with a graph metric of pathology spread (i.e., node-strength) in tauopathies (r= 0.60,p< 0.03) but not in TDP-43 proteinopathies (r= 0.03,p= 0.9). Finally, we found mediation effects for WM pathology on the association between anterior and posterior GM pathology in FTLD-Tau but not in FTLD-TDP. These data suggest distinct tau and TDP-43 proteinopathies may have divergent patterns of cellular propagation in GM and WM. More specifically, axonal spread may be more influential in FTLD-Tau progression. Network analyses of digital histopathological measurements can inform models of disease progression of cellular degeneration in the human brain.SIGNIFICANCE STATEMENTIn this study, we uniquely perform two complimentary computational approaches to model and contrast microscopic disease progression between common frontotemporal lobar degeneration (FTLD) proteinopathy subtypes with similar clinical syndromes during life. Our models suggest white matter (WM) pathology influences cortical spread of disease in tauopathies that is less evident in TDP-43 proteinopathies. These data support the hypothesis that there are neuropathologic signatures of cellular degeneration within neurocognitive networks for specific protienopathies. These distinctive patterns of cellular pathology can guide future efforts to develop tissue-sensitive imaging and biological markers with diagnostic and prognostic utility for FTLD. Moreover, our novel computational approach can be used in future work to model various neurodegenerative disorders with mixed proteinopathy within the human brain connectome.

Published

2022

10. Antemortem network analysis of spreading pathology in autopsy-confirmed frontotemporal degeneration

Author

Min Chen, Sarah Burke, Christopher A Olm, David J Irwin, Lauren Massimo, Edward B Lee, John Q Trojanowski, James C Gee, and Murray Grossman

Subjects

Cellular and Molecular Neuroscience, Psychiatry and Mental health, Neurology, Biological Psychiatry

Abstract

Despite well-articulated hypotheses of spreading pathology in animal models of neurodegenerative disease, the basis for spreading neurodegenerative pathology in humans has been difficult to ascertain. In this study, we used graph theoretic analyses of structural networks in antemortem, multimodal MRI from autopsy-confirmed cases to examine spreading pathology in sporadic frontotemporal lobar degeneration. We defined phases of progressive cortical atrophy on T1-weighted MRI using a published algorithm in autopsied frontotemporal lobar degeneration with tau inclusions or with transactional DNA binding protein of ∼43 kDa inclusions. We studied global and local indices of structural networks in each of these phases, focusing on the integrity of grey matter hubs and white matter edges projecting between hubs. We found that global network measures are compromised to an equal degree in patients with frontotemporal lobar degeneration with tau inclusions and frontotemporal lobar degeneration-transactional DNA binding protein of ∼43 kDa inclusions compared to healthy controls. While measures of local network integrity were compromised in both frontotemporal lobar degeneration with tau inclusions and frontotemporal lobar degeneration-transactional DNA binding protein of ∼43 kDa inclusions, we discovered several important characteristics that distinguished between these groups. Hubs identified in controls were degraded in both patient groups, but degraded hubs were associated with the earliest phase of cortical atrophy (i.e. epicentres) only in frontotemporal lobar degeneration with tau inclusions. Degraded edges were significantly more plentiful in frontotemporal lobar degeneration with tau inclusions than in frontotemporal lobar degeneration-transactional DNA binding protein of ∼43 kDa inclusions, suggesting that the spread of tau pathology involves more significant white matter degeneration. Weakened edges were associated with degraded hubs in frontotemporal lobar degeneration with tau inclusions more than in frontotemporal lobar degeneration-transactional DNA binding protein of ∼43 kDa inclusions, particularly in the earlier phases of the disease, and phase-to-phase transitions in frontotemporal lobar degeneration with tau inclusions were characterized by weakened edges in earlier phases projecting to diseased hubs in subsequent phases of the disease. When we examined the spread of pathology from a region diseased in an earlier phase to physically adjacent regions in subsequent phases, we found greater evidence of disease spreading to adjacent regions in frontotemporal lobar degeneration-transactional DNA binding protein of ∼43 kDa inclusions than in frontotemporal lobar degeneration with tau inclusions. We associated evidence of degraded grey matter hubs and weakened white matter edges with quantitative measures of digitized pathology from direct observations of patients’ brain samples. We conclude from these observations that the spread of pathology from diseased regions to distant regions via weakened long-range edges may contribute to spreading disease in frontotemporal dementia-tau, while spread of pathology to physically adjacent regions via local neuronal connectivity may play a more prominent role in spreading disease in frontotemporal lobar degeneration-transactional DNA binding protein of ∼43 kDa inclusions.

Published

2023

11. ApoJ/Clusterin concentrations are determinants of cerebrospinal fluid cholesterol efflux capacity and reduced levels are associated with Alzheimer’s disease

Author

Yi-An Ko, Jeffrey T. Billheimer, Nicholas N. Lyssenko, Alexandra Kueider-Paisley, David A. Wolk, Steven E. Arnold, Yuk Yee Leung, Leslie M. Shaw, John Q. Trojanowski, Rima F. Kaddurah-Daouk, Mitchel A. Kling, and Daniel J. Rader

Subjects

Neurology, Cognitive Neuroscience, Neurology (clinical)

Abstract

Background Alzheimer’s disease (AD) shares risk factors with cardiovascular disease (CVD) and dysregulated cholesterol metabolism is a mechanism common to both diseases. Cholesterol efflux capacity (CEC) is an ex vivo metric of plasma high-density lipoprotein (HDL) function and inversely predicts incident CVD independently of other risk factors. Cholesterol pools in the central nervous system (CNS) are largely separate from those in blood, and CNS cholesterol excess may promote neurodegeneration. CEC of cerebrospinal fluid (CSF) may be a useful measure of CNS cholesterol trafficking. We hypothesized that subjects with AD and mild cognitive impairment (MCI) would have reduced CSF CEC compared with Cognitively Normal (CN) and that CSF apolipoproteins apoA-I, apoJ, and apoE might have associations with CSF CEC. Methods We retrieved CSF and same-day ethylenediaminetetraacetic acid (EDTA) plasma from 108 subjects (40 AD; 18 MCI; and 50 CN) from the Center for Neurodegenerative Disease Research biobank at the Perelman School of Medicine, University of Pennsylvania. For CSF CEC assays, we used N9 mouse microglial cells and SH-SY5Y human neuroblastoma cells, and the corresponding plasma assay used J774 cells. Cells were labeled with [3H]-cholesterol for 24 h, had ABCA1 expression upregulated for 6 h, were exposed to 33 μl of CSF, and then were incubated for 2.5 h. CEC was quantified as percent [3H]-cholesterol counts in medium of total counts medium+cells, normalized to a pool sample. ApoA-I, ApoJ, ApoE, and cholesterol were also measured in CSF. Results We found that CSF CEC was significantly lower in MCI compared with controls and was poorly correlated with plasma CEC. CSF levels of ApoJ/Clusterin were also significantly lower in MCI and were significantly associated with CSF CEC. While CSF ApoA-I was also associated with CSF CEC, CSF ApoE had no association with CSF CEC. CSF CEC is significantly and positively associated with CSF Aβ. Taken together, ApoJ/Clusterin may be an important determinant of CSF CEC, which in turn could mitigate risk of MCI and AD risk by promoting cellular efflux of cholesterol or other lipids. In contrast, CSF ApoE does not appear to play a role in determining CSF CEC.

Published

2022

12. Deep learning pipeline for cortical gray matter segmentation and thickness analysis in Ultra High Resolution T2w 7 Tesla Ex vivo MRI across neurodegenerative diseases reveals associations with underlying neuropathology

Author

Pulkit Khandelwal, Shokufeh Sadaghiani, Eunice Chung, Sydney A Lim, Michael Tran Duong, Sadhana Ravikumar, Sanaz Arezoumandan, Claire Peterson, Madigan L Bedard, Noah Capp, Ranjit Ittyerah, Elyse Migdal, Grace Choi, Emily Kopp, Bridget Loja Patino, Eusha Hasan, Jiacheng Li, Karthik Prabhakaran, Gabor Mizsei, Marianna Gabrielyan, Theresa Schuck, John Robinson, Daniel T Ohm, Eddie B Lee, John Q Trojanowski, Corey T McMillan, Murray Grossman, David J. Irwin, Dylan M Tisdall, Sandhitsu R. Das, Laura EM Wisse, David A. Wolk, and Paul A. Yushkevich

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Neurology (clinical), Geriatrics and Gerontology

Published

2022

13. Plasma GFAP:NfL discriminates FTLD‐tau from FTLD‐TDP

Author

Katheryn A Q Cousins, Leslie M. Shaw, Alice Chen‐Plotkin, Eddie B Lee, John Q Trojanowski, Vivianna M Van Deerlin, Corey T McMillan, Murray Grossman, and David J. Irwin

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Neurology (clinical), Geriatrics and Gerontology

Published

2022

14. Linking histology to post‐mortem 7T MRI measures of neurodegeneration

Author

Shokufeh Sadaghiani, Sadhana Ravikumar, Ranjit Ittyerah, Sydney A Lim, Eunice Chung, Madigan L Bedard, Long Xie, Sandhitsu R. Das, Theresa Schuck, Murray Grossman, Eddie B Lee, Dylan M Tisdall, Karthik Prabhakaran, John A. Detre, Gabor Mizsei, John Q Trojanowski, David J. Irwin, Laura EM Wisse, David A. Wolk, and Paul A. Yushkevich

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Neurology (clinical), Geriatrics and Gerontology

Published

2022

15. Deep Learning for Ultra High Resolution T2‐weighted 7 Tesla Ex vivo Magnetic Resonance Imaging Reveals Differential Subcortical Atrophy across Neurodegenerative Diseases

Author

Pulkit Khandelwal, Michael Tran Duong, Eunice Chung, Shokufeh Sadaghiani, Sydney A Lim, Sadhana Ravikumar, Sanaz Arezoumandan, Claire Peterson, Madigan L Bedard, Noah Capp, Ranjit Ittyerah, Elyse Migdal, Grace Choi, Emily Kopp, Bridget Loja Patino, Eusha Hasan, Jiacheng Li, Karthik Prabhakaran, Gabor Mizsei, Marianna Gabrielyan, Theresa Schuck, John L. Robinson, Daniel T Ohm, Ilya M. Nasrallah, Eddie B Lee, John Q Trojanowski, Corey T McMillan, Murray Grossman, David J. Irwin, Dylan M Tisdall, Sandhitsu R. Das, Laura EM Wisse, David A. Wolk, and Paul A. Yushkevich

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Neurology (clinical), Geriatrics and Gerontology

Published

2022

16. Tau‐Neurodegeneration mismatch reveals vulnerability and resilience in Alzheimer’s continuum and Non‐Alzheimer’s pathophysiology

Author

Xueying Lyu, Michael Tran Duong, Long Xie, Hayley Richardson, Robin de Flores, Michael DiCalogero, Corey T McMillan, John Robinson, John Q Trojanowski, Murray Grossman, Eddie B Lee, David J. Irwin, Brad C. Dickerson, Sharon X Xie, Ilya M. Nasrallah, Paul A. Yushkevich, David A. Wolk, and Sandhitsu R. Das

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Neurology (clinical), Geriatrics and Gerontology

Published

2022

17. Combining high‐resolution ex vivo MRI and histopathology to identify medial temporal lobe atrophy patterns specific to tau pathology in Alzheimer’s Disease

Author

Sadhana Ravikumar, Amanda Denning, Sydney A Lim, Eunice Chung, Ranjit Ittyerah, Laura EM Wisse, Long Xie, Sandhitsu R. Das, John Robinson, Theresa Schuck, Murray Grossman, Eddie B Lee, Dylan M Tisdall, Gabor Mizsei, Emilio Artacho‐Perula, Maria Mercedes Iniguez de Onzono Martin, Mar Arroyo Jimenez, Monica Munoz, Francisco Javier Molina Romero, Pilar Marcos Rabal, Sandra Cebada Sanchez, Jose Carlos Delgado Gonzalez, Rosa Prieto, Marta Corcoles Parada, David J. Irwin, John Q Trojanowski, David A. Wolk, Ricardo Insausti, and Paul A. Yushkevich

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Neurology (clinical), Geriatrics and Gerontology

Published

2022

18. Genome-wide association study and functional validation implicates JADE1 in tauopathy

Author

John F. Crary, Katia de Paiva Lopes, Bradley T. Hyman, Manav Kapoor, Gloriia Novikova, Jonathan D. Glass, Valeriy Borukov, Hadley Walsh, Erin E. Franklin, Johannes Attems, Sara Shuldberg, Shea J. Andrews, Thomas J. Montine, Julie A. Schneider, Jonathan D. Cherry, C. Dirk Keene, Towfique Raj, Charles L. White, Thor D. Stein, Evan Udine, Gai Ayalon, Thao Pham, Maria M. Corrada, Weijing Tang, Ann C. McKee, Bess Frost, Marco M. Hefti, Qinwen Mao, Lei Yu, Patrick R. Hof, Peter T. Nelson, Elias M. Gonzalez, Alan E. Renton, Corey T. McMillan, Jack Humphrey, Natalia Han, Margaret E. Flanagan, SoongHo Kim, Etty Cortes, Megan A. Iida, Inma Cobos, Jeff Metcalf, Sandra Weintraub, Julie Hunkapiller, Diana K. Dangoor, Robert A. Rissman, Marcos Otero-Garcia, John Q. Trojanowski, Dushyant P. Purohit, Caitlin S. Latimer, Marla Gearing, Claudia H. Kawas, Kathryn R. Bowles, Wayne W. Poon, Brian Fulton-Howard, Edoardo Marcora, Alison Goate, Alicia Casella, Tushar Bhangale, Richard J. Perrin, Herbert T. Cohen, Bahar Salehi, Gabor G. Kovacs, Andy F. Teich, Mary Sano, Jamie M. Walker, Dennis W. Dickson, Randy Woltjer, Kristen Whitney, M.-Marsel Mesulam, Ricardo Assunção Vialle, Peter Fischer, Kurt Farrell, Jean-Paul Vonsattel, Cheick T. Sissoko, Vahram Haroutunian, Sam Gandy, Mirjam I. Lutz, Matthew P. Frosch, Nigel J. Cairns, Melissa E. Murray, Robert R. Graham, David A. Wolk, Juan C. Troncoso, Garrett Wong, Julia Kofler, Edward B. Lee, Timothy E. Richardson, and Thomas G. Beach

Subjects

Male, Aging, Locus (genetics), Single-nucleotide polymorphism, Genome-wide association study, Biology, Polymorphism, Single Nucleotide, Article, Pathology and Forensic Medicine, Progressive supranuclear palsy, Cohort Studies, Cellular and Molecular Neuroscience, medicine, Animals, Humans, Aged, Genetic association, Aged, 80 and over, Homeodomain Proteins, Tumor Suppressor Proteins, Neurofibrillary tangle, Middle Aged, medicine.disease, Molecular biology, Tauopathies, Drosophila, Female, Neurology (clinical), Tauopathy, Alzheimer's disease, Genome-Wide Association Study

Abstract

Primary age-related tauopathy (PART) is a neurodegenerative pathology with features distinct from but also overlapping with Alzheimer disease (AD). While both exhibit Alzheimer-type temporal lobe neurofibrillary degeneration alongside amnestic cognitive impairment, PART develops independently of amyloid-β (Aβ) plaques. The pathogenesis of PART is not known, but evidence suggests an association with genes that promote tau pathology and others that protect from Aβ toxicity. Here, we performed a genetic association study in an autopsy cohort of individuals with PART (n = 647) using Braak neurofibrillary tangle stage as a quantitative trait. We found some significant associations with candidate loci associated with AD (SLC24A4, MS4A6A, HS3ST1) and progressive supranuclear palsy (MAPT and EIF2AK3). Genome-wide association analysis revealed a novel significant association with a single nucleotide polymorphism on chromosome 4 (rs56405341) in a locus containing three genes, including JADE1 which was significantly upregulated in tangle-bearing neurons by single-soma RNA-seq. Immunohistochemical studies using antisera targeting JADE1 protein revealed localization within tau aggregates in autopsy brains with four microtubule-binding domain repeats (4R) isoforms and mixed 3R/4R, but not with 3R exclusively. Co-immunoprecipitation in post-mortem human PART brain tissue revealed a specific binding of JADE1 protein to four repeat tau lacking N-terminal inserts (0N4R). Finally, knockdown of the Drosophila JADE1 homolog rhinoceros (rno) enhanced tau-induced toxicity and apoptosis in vivo in a humanized 0N4R mutant tau knock-in model, as quantified by rough eye phenotype and terminal deoxynucleotidyl transferase dUTP nick end-labeling (TUNEL) in the fly brain. Together, these findings indicate that PART has a genetic architecture that partially overlaps with AD and other tauopathies and suggests a novel role for JADE1 as a modifier of neurofibrillary degeneration.

Published

2021

19. Contribution of Alzheimer's biomarkers and risk factors to cognitive impairment and decline across the Alzheimer's disease continuum

Author

William J. Jagust, Leslie M. Shaw, Andrew J. Saykin, John Q. Trojanowski, Alzheimer’s Disease Neuroimaging Initiative, Ronald C. Petersen, Dallas P. Veitch, Daniel Weintraub, Clifford R. Jack, Michael W. Weiner, Paul S. Aisen, Zeynep Demir, and Duygu Tosun

Subjects

Oncology, Apolipoprotein E, medicine.medical_specialty, Epidemiology, Amyloid beta, tau Proteins, Cellular and Molecular Neuroscience, Atrophy, Developmental Neuroscience, Alzheimer Disease, Risk Factors, Internal medicine, medicine, Humans, Dementia, Cognitive Dysfunction, Cognitive decline, Aged, Amyloid beta-Peptides, biology, business.industry, Health Policy, Neurodegeneration, Brain, Cognition, medicine.disease, Hyperintensity, Psychiatry and Mental health, Cross-Sectional Studies, Positron-Emission Tomography, biology.protein, Neurology (clinical), Geriatrics and Gerontology, business, Biomarkers

Abstract

Introduction Amyloid beta (Aβ), tau, and neurodegeneration jointly with the Alzheimer's disease (AD) risk factors affect the severity of clinical symptoms and disease progression. Methods Within 248 Aβ-positive elderly with and without cognitive impairment and dementia, partial least squares structural equation pathway modeling was used to assess the direct and indirect effects of imaging biomarkers (global Aβ-positron emission tomography [PET] uptake, regional tau-PET uptake, and regional magnetic resonance imaging-based atrophy) and risk-factors (age, sex, education, apolipoprotein E [APOE], and white-matter lesions) on cross-sectional cognitive impairment and longitudinal cognitive decline. Results Sixteen percent of variance in cross-sectional cognitive impairment was accounted for by Aβ, 46% to 47% by tau, and 25% to 29% by atrophy, although 53% to 58% of total variance in cognitive impairment was explained by incorporating mediated and direct effects of AD risk factors. The Aβ-tau-atrophy pathway accounted for 50% to 56% of variance in longitudinal cognitive decline while Aβ, tau, and atrophy independently explained 16%, 46% to 47%, and 25% to 29% of the variance, respectively. Discussion These findings emphasize that treatments that remove Aβ and completely stop downstream effects on tau and neurodegeneration would only be partially effective in slowing of cognitive decline or reversing cognitive impairment.

Published

2021

20. Using the Alzheimer's Disease Neuroimaging Initiative to improve early detection, diagnosis, and treatment of Alzheimer's disease

Author

Paul S. Aisen, Michael W. Weiner, Danielle J Harvey, William J. Jagust, John Q. Trojanowski, Robert C. Green, Alzheimer’s Disease Neuroimaging Initiative, Susan M. Landau, Arthur W. Toga, Leslie M. Shaw, Ronald C. Petersen, Monica Rivera-Mindt, Duygu Tosun, Richard J. Perrin, John C. Morris, Laurel A. Beckett, Andrew J. Saykin, Clifford R. Jack, Ozioma C. Okonkwo, Dallas P. Veitch, and Charles DeCarli

Subjects

Oncology, Aging, Epidemiology, Disease, Neurodegenerative, Alzheimer's Disease, tau, screening and diagnosis, biology, Health Policy, AV1541 tau positron emission tomography, amyloid, plasma biomarker, Detection, Psychiatry and Mental health, Neurological, Cohort, Disease Progression, Biomedical Imaging, Alzheimer's Disease Neuroimaging Initiative, medicine.medical_specialty, Amyloid beta, Clinical Sciences, Neuroimaging, tau Proteins, Cellular and Molecular Neuroscience, disease progression, mild cognitive impairment, Developmental Neuroscience, Alzheimer Disease, Internal medicine, mental disorders, Acquired Cognitive Impairment, medicine, Humans, Cognitive Dysfunction, Amyloid beta-Peptides, Vascular disease, business.industry, Prevention, Neurosciences, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), medicine.disease, Brain Disorders, 4.1 Discovery and preclinical testing of markers and technologies, Biomarker (cell), Clinical trial, Geriatrics, biology.protein, Dementia, Neurology (clinical), Geriatrics and Gerontology, business, Biomarkers

Abstract

INTRODUCTION The Alzheimer's Disease Neuroimaging Initiative (ADNI) has accumulated 15 years of clinical, neuroimaging, cognitive, biofluid biomarker and genetic data, and biofluid samples available to researchers, resulting in more than 3500 publications. This review covers studies from 2018 to 2020. METHODS We identified 1442 publications using ADNI data by conventional search methods and selected impactful studies for inclusion. RESULTS Disease progression studies supported pivotal roles for regional amyloid beta (Aβ) and tau deposition, and identified underlying genetic contributions to Alzheimer's disease (AD). Vascular disease, immune response, inflammation, resilience, and sex modulated disease course. Biologically coherent subgroups were identified at all clinical stages. Practical algorithms and methodological changes improved determination of Aβ status. Plasma Aβ, phosphorylated tau181, and neurofilament light were promising noninvasive biomarkers. Prognostic and diagnostic models were externally validated in ADNI but studies are limited by lack of ethnocultural cohort diversity. DISCUSSION ADNI has had a profound impact in improving clinical trials for AD.

Published

2021

21. Associations of phosphorylated tau pathology with whole-hemisphere ex vivo morphometry in 7 tesla MRI

Author

Shokufeh Sadaghiani, Winifred Trotman, Sydney A. Lim, Eunice Chung, Ranjit Ittyerah, Sadhana Ravikumar, Pulkit Khandelwal, Karthik Prabhakaran, Madigan L. Lavery, Daniel T. Ohm, Marianna Gabrielyan, Sandhitsu R. Das, Theresa Schuck, Noah Capp, Claire S. Peterson, Elyse Migdal, Emilio Artacho‐Pérula, María del Mar Arroyo Jiménez, Maria del Pilar Marcos Rabal, Sandra Cebada Sánchez, Carlos de la Rosa Prieto, Marta Córcoles Parada, Ricardo Insausti, John L. Robinson, Corey McMillan, Murray Grossman, Edward B. Lee, John A. Detre, Sharon X. Xie, John Q. Trojanowski, M. Dylan Tisdall, Laura E. M. Wisse, David J. Irwin, David A. Wolk, and Paul A. Yushkevich

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Neurology (clinical), Geriatrics and Gerontology

Abstract

Neurodegenerative disorders are associated with different pathologies that often co-occur but cannot be measured specifically with in vivo methods.Thirty-three brain hemispheres from donors with an Alzheimer's disease (AD) spectrum diagnosis underwent T2-weighted magnetic resonance imaging (MRI). Gray matter thickness was paired with histopathology from the closest anatomic region in the contralateral hemisphere.Partial Spearman correlation of phosphorylated tau and cortical thickness with TAR DNA-binding protein 43 (TDP-43) and α-synuclein scores, age, sex, and postmortem interval as covariates showed significant relationships in entorhinal and primary visual cortices, temporal pole, and insular and posterior cingulate gyri. Linear models including Braak stages, TDP-43 and α-synuclein scores, age, sex, and postmortem interval showed significant correlation between Braak stage and thickness in the parahippocampal gyrus, entorhinal cortex, and Broadman area 35.We demonstrated an association of measures of AD pathology with tissue loss in several AD regions despite a limited range of pathology in these cases.Neurodegenerative disorders are associated with co-occurring pathologies that cannot be measured specifically with in vivo methods. Identification of the topographic patterns of these pathologies in structural magnetic resonance imaging (MRI) may provide probabilistic biomarkers. We demonstrated the correlation of the specific patterns of tissue loss from ex vivo brain MRI with underlying pathologies detected in postmortem brain hemispheres in patients with Alzheimer's disease (AD) spectrum disorders. The results provide insight into the interpretation of in vivo structural MRI studies in patients with AD spectrum disorders.

Published

2022

22. Synapsin-caveolin-1 gene therapy preserves neuronal and synaptic morphology and prevents neurodegeneration in a mouse model of AD

Author

Isabella C. Kelly, Mehul Dhanani, John Q. Trojanowski, Kimberly Zhou, Sonia Podvin, Steve L. Wagner, Atsushi Miyanohara, Shanshan Wang, Piyush M. Patel, Tong Zhang, Vivian Hook, Alexander M. Kleschevnikov, Phuong Nguyen, Joseph Leem, Natalia Kleschevnikov, Brian P. Head, David M. Roth, Hemal H. Patel, and Paul Savchenko

Subjects

0301 basic medicine, Aging, caveolin-1, Transgene, Hippocampus, PSAPP, QH426-470, Neurodegenerative, membrane lipid raft, Biology, Alzheimer's Disease, 03 medical and health sciences, Myelin, 0302 clinical medicine, Neuroplasticity, Acquired Cognitive Impairment, Genetics, medicine, 2.1 Biological and endogenous factors, Aetiology, Molecular Biology, QH573-671, Neurodegeneration, Neurosciences, synaptic ultrastructure, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Synapsin, medicine.disease, gene therapy, Brain Disorders, Astrogliosis, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Neurological, Caveolin 1, Molecular Medicine, Original Article, Dementia, Cytology, Alzheimer’s disease, Neuroscience, MLRs

Abstract

Alzheimer’s disease (AD) is the most common form of neurodegeneration and cognitive dysfunction in the elderly. Identifying molecular signals that mitigate and reverse neurodegeneration in AD may be exploited therapeutically. Transgenic AD mice (PSAPP) exhibit learning and memory deficits at 9 and 11 months, respectively, with associated decreased expression of caveolin-1 (Cav-1), a membrane/lipid raft (MLR) scaffolding protein necessary for synaptic and neuroplasticity. Neuronal-targeted gene therapy using synapsin-Cav-1 cDNA (SynCav1) was delivered to the hippocampus of PSAPP mice at 3 months using adeno-associated virus serotype 9 (AAV9). Bilateral SynCav1 gene therapy was able to preserve MLRs profile, learning and memory, hippocampal dendritic arbor, synaptic ultrastructure, and axonal myelin content in 9- and 11-month PSAPP mice, independent of reducing toxic amyloid deposits and astrogliosis. Our data indicate that SynCav1 gene therapy may be an option for AD and potentially in other forms of neurodegeneration of unknown etiology., Graphical abstract, The findings demonstrate that regardless of the etiology of the neuropathology, SynCav1 may be exploited to treat sporadic conditions or to be used in combination with already existing drugs or biologics designed to target known monogenic candidates linked to other neurodegenerative conditions (AD, ALS, MS).

Published

2021

23. Isoform-specific patterns of tau burden and neuronal degeneration in MAPT-associated frontotemporal lobar degeneration

Author

Lucia A A, Giannini, Daniel T, Ohm, Annemieke J M, Rozemuller, Laynie, Dratch, EunRan, Suh, Vivianna M, van Deerlin, John Q, Trojanowski, Edward B, Lee, John C, van Swieten, Murray, Grossman, Harro, Seelaar, and David J, Irwin

Subjects

Neurons, Tauopathies, Frontotemporal Dementia, Humans, Protein Isoforms, tau Proteins, Frontotemporal Lobar Degeneration

Abstract

Frontotemporal lobar degeneration with MAPT pathogenic variants (FTLD-MAPT) has heterogeneous tau pathological inclusions postmortem, consisting of three-repeat (3R) or four-repeat (4R) tau isoforms, or a combination (3R + 4R). Here, we studied grey matter tau burden, its relation to neuronal degeneration, and regional patterns of pathology in different isoform groups of FTLD-MAPT. We included 38 FTLD-MAPT autopsy cases with 10 different MAPT pathogenic variants, grouped based on predominant tau isoform(s). In up to eleven regions (ten cortical and one striatal), we quantified grey matter tau burden using digital histopathological analysis and assigned semi-quantitative ratings for neuronal degeneration (i.e. 0-4) and separate burden of glial and neuronal tau inclusions (i.e. 0-3). We used mixed modelling to compare pathology measures (1) across the entire cohort and (2) within isoform groups. In the total cohort, tau burden and neuronal degeneration were positively associated and most severe in the anterior temporal, anterior cingulate and transentorhinal cortices. Isoform groups showed distinctive features of tau burden and neuronal degeneration. Across all regions, the 3R isoform group had lower tau burden compared to the 4R group (p = 0.008), while at the same time showing more severe neuronal degeneration than the 4R group (p = 0.002). The 3R + 4R group had an intermediate profile with relatively high tau burden along with relatively severe neuronal degeneration. Neuronal tau inclusions were most frequent in the 4R group (p 0.001 vs. 3R), while cortical glial tau inclusions were most frequent in the 3R + 4R and 4R groups (p ≤ 0.009 vs. 3R). Regionally, neuronal degeneration was consistently most severe in the anterior temporal cortex within each isoform group. In contrast, the regions with the highest tau burden differed in isoform groups (3R: striatum; 3R + 4R: striatum, inferior parietal lobule, middle frontal cortex, anterior cingulate cortex; 4R: transentorhinal cortex, anterior temporal cortex, fusiform gyrus). We conclude that FTLD-MAPT isoform groups show distinctive features of overall neuronal degeneration and regional tau burden, but all share pronounced anterior temporal neuronal degeneration. These data suggest that distinct isoform-related mechanisms of genetic tauopathies, with slightly divergent tau distribution, may share similar regional vulnerability to neurodegeneration within the frontotemporal paralimbic networks.

Published

2022

24. Cognitive Profile and Markers of Alzheimer Disease–Type Pathology in Patients With Lewy Body Dementias

Author

Andrew Siderowf, Nabila Dahodwala, Murray Grossman, Andres Deik, James F. Morley, Leslie M. Shaw, Meredith Spindler, David J. Irwin, Erica Howard, Thomas F. Tropea, John Q. Trojanowski, Naomi Nevler, John E. Duda, David A. Wolk, Katheryn A.Q. Cousins, Sanjeev N. Vaishnavi, Dawn Mechanic-Hamilton, Alice Chen-Plotkin, Sanjana Shellikeri, Daniel Weintraub, and Katya Rascovsky

Subjects

Lewy Body Disease, Male, 0301 basic medicine, medicine.medical_specialty, tau Proteins, Gastroenterology, Article, Amyloid beta-Protein Precursor, 03 medical and health sciences, 0302 clinical medicine, Alzheimer Disease, Internal medicine, mental disorders, medicine, Memory span, Humans, Dementia, Effects of sleep deprivation on cognitive performance, Aged, Aged, 80 and over, Language Tests, Lewy body, business.industry, Dementia with Lewy bodies, Neuropsychology, Brain, Middle Aged, medicine.disease, 030104 developmental biology, Boston Naming Test, Female, Neurology (clinical), Alzheimer's disease, business, hormones, hormone substitutes, and hormone antagonists, Biomarkers, 030217 neurology & neurosurgery

Abstract

ObjectiveTo determine whether patients with Lewy body dementia (LBD) with likely Alzheimer disease (AD)–type copathology are more impaired on confrontation naming than those without likely AD-type copathology.MethodsWe selected 57 patients with LBD (dementia with Lewy bodies [DLB], n = 38; Parkinson disease dementia [PDD], n = 19) with available AD CSF biomarkers and neuropsychological data. CSF β-amyloid1-42 (Aβ42), phosphorylated-tau (p-tau), and total-tau (t-tau) concentrations were measured. We used an autopsy-validated CSF cut point (t-tau:Aβ42 ratio > 0.3, n = 43), or autopsy data when available (n = 14), to categorize patients as having LBD with (LBD + AD, n = 26) and without (LBD − AD, n = 31) likely AD-type copathology. Analysis of covariance tested between-group comparisons across biologically defined groups (LBD + AD, LBD − AD) and clinical phenotypes (DLB, PDD) on confrontation naming (30-item Boston Naming Test [BNT]), executive abilities (letter fluency [LF], reverse digit span [RDS]), and global cognition (Mini-Mental State Examination [MMSE]), with adjustment for age at dementia onset, time from dementia onset to test date, and time from CSF to test date. Spearman correlation related cognitive performance to CSF analytes.ResultsPatients with LBD + AD performed worse on BNT than patients with LBD − AD (F = 4.80, p = 0.03); both groups performed similarly on LF, RDS, and MMSE (all p > 0.1). Clinically defined PDD and DLB groups did not differ in performance on any of these measures (all p > 0.05). A correlation across all patients showed that BNT score was negatively associated with CSF t-tau (ρ = −0.28, p < 0.05) and p-tau (ρ = −0.26, p = 0.05) but not Aβ42 (p > 0.1).ConclusionMarkers of AD-type copathology are implicated in impaired language performance in LBD. Biologically based classification of LBD may be advantageous over clinically defined syndromes to elucidate clinical heterogeneity.

Published

2021

25. Neuropathological consensus criteria for the evaluation of Lewy pathology in post-mortem brains: a multi-centre study

Author

Tuomo Polvikoski, Laura Parkkinen, Lea T. Grinberg, Peter T. Nelson, Steve M. Gentleman, Johannes Attems, John Q. Trojanowski, Jon B. Toledo, Edward B. Lee, Ellen Gelpi, Kirsty E. McAleese, Colin Smith, Gabor G. Kovacs, Seth Love, Manuela Neumann, Ian G. McKeith, Lauren Walker, Glenda M. Halliday, Beata Sikorska, Kurt A. Jellinger, Tibor Hortobágyi, Dietmar Rudolf Thal, and Parkinson's UK

Subjects

Male, INVOLVEMENT, Aging, ALPHA-SYNUCLEIN, Consensus criteria, Neurodegenerative, Audiology, Alzheimer's Disease, GUIDELINES, PARKINSONS-DISEASE, pathology [Brain], 80 and over, Pathology, 2.1 Biological and endogenous factors, Cluster Analysis, Aetiology, Multi centre, ALZHEIMERS, Observer Variation, Brain Mapping, Parkinson's Disease, CLINICAL DIAGNOSTIC-CRITERIA, DEMENTIA, Brain, Parkinson Disease, Neurological, Female, Autopsy, Alzheimer's disease, diagnosis [Lewy Body Disease], Life Sciences & Biomedicine, medicine.medical_specialty, Consensus, Clinical Sciences, Clinical Neurology, Lewy body disease, Pathology and Forensic Medicine, Cellular and Molecular Neuroscience, Alzheimer Disease, classification [Lewy Body Disease], Lewy pathology, Acquired Cognitive Impairment, MANAGEMENT, medicine, Humans, Dementia, ddc:610, Staging system, Aged, pathology [Lewy Bodies], Original Paper, Science & Technology, Neurology & Neurosurgery, Lewy body, business.industry, Neurosciences, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), pathology [Lewy Body Disease], Reproducibility of Results, 1103 Clinical Sciences, COGNITIVE IMPAIRMENT, medicine.disease, Diagnostic neuropathology, Brain Disorders, Lewy Bodies, Neurosciences & Neurology, Neurology (clinical), 1109 Neurosciences, business, SYSTEM

Abstract

Currently, the neuropathological diagnosis of Lewy body disease (LBD) may be stated according to several staging systems, which include the Braak Lewy body stages (Braak), the consensus criteria by McKeith and colleagues (McKeith), the modified McKeith system by Leverenz and colleagues (Leverenz), and the Unified Staging System by Beach and colleagues (Beach). All of these systems use semi-quantitative scoring (4- or 5-tier scales) of Lewy pathology (LP; i.e., Lewy bodies and Lewy neurites) in defined cortical and subcortical areas. While these systems are widely used, some suffer from low inter-rater reliability and/or an inability to unequivocally classify all cases with LP. To address these limitations, we devised a new system, the LP consensus criteria (LPC), which is based on the McKeith system, but applies a dichotomous approach for the scoring of LP (i.e., “absent” vs. “present”) and includes amygdala-predominant and olfactory-only stages. α-Synuclein-stained slides from brainstem, limbic system, neocortex, and olfactory bulb from a total of 34 cases with LP provided by the Newcastle Brain Tissue Resource (NBTR) and the University of Pennsylvania brain bank (UPBB) were scanned and assessed by 16 raters, who provided diagnostic categories for each case according to Braak, McKeith, Leverenz, Beach, and LPC systems. In addition, using LP scores available from neuropathological reports of LP cases from UPBB (n = 202) and NBTR (n = 134), JT (UPBB) and JA (NBTR) assigned categories according to all staging systems to these cases. McKeith, Leverenz, and LPC systems reached good (Krippendorff’s α ≈ 0.6), while both Braak and Beach systems had lower (Krippendorff’s α ≈ 0.4) inter-rater reliability, respectively. Using the LPC system, all cases could be unequivocally classified by the majority of raters, which was also seen for 97.1% when the Beach system was used. However, a considerable proportion of cases could not be classified when using Leverenz (11.8%), McKeith (26.5%), or Braak (29.4%) systems. The category of neocortical LP according to the LPC system was associated with a 5.9 OR (p p = 0.0001) in the 202 UPBB cases. We established that the LPC system has good reproducibility and allows classification of all cases into distinct categories. We expect that it will be reliable and useful in routine diagnostic practice and, therefore, suggest that it should be the standard future approach for the basic post-mortem evaluation of LP.

Published

2021

26. Slow motor neurons resist pathological TDP-43 and mediate motor recovery in the rNLS8 model of amyotrophic lateral sclerosis

Author

Seong Kwon Hur, Mandana Hunter, Myrna A. Dominique, Madona Farag, Dejania Cotton-Samuel, Tahiyana Khan, John Q. Trojanowski, Krista J. Spiller, and Virginia M.-Y. Lee

Subjects

DNA-Binding Proteins, Motor Neurons, Mice, Cellular and Molecular Neuroscience, TDP-43 Proteinopathies, Amyotrophic Lateral Sclerosis, Animals, Humans, Mice, Transgenic, Neurology (clinical), Pathology and Forensic Medicine

Abstract

In the intermediate stages of amyotrophic lateral sclerosis (ALS), surviving motor neurons (MNs) that show intrinsic resistance to TDP-43 proteinopathy can partially compensate for the loss of their more disease-susceptible counterparts. Elucidating the mechanisms of this compensation may reveal approaches for attenuating motor impairment in ALS patients. In the rNLS8 mouse model of ALS-like pathology driven by doxycycline-regulated neuronal expression of human TDP-43 lacking a nuclear localization signal (hTDP-43ΔNLS), slow MNs are more resistant to disease than fast-fatigable (FF) MNs and can mediate recovery following transgene suppression. In the present study, we used a viral tracing strategy to show that these disease-resistant slow MNs sprout to reinnervate motor endplates of adjacent muscle fibers vacated by degenerated FF MNs. Moreover, we found that neuromuscular junctions within fast-twitch skeletal muscle (tibialis anterior, TA) reinnervated by SK3-positive slow MNs acquire resistance to axonal dieback when challenged with a second course of hTDP-43ΔNLS pathology. The selective resistance of reinnervated neuromuscular junctions was specifically induced by the unique pattern of reinnervation following TDP-43-induced neurodegeneration, as recovery from unilateral sciatic nerve crush did not produce motor units resistant to subsequent hTDP-43ΔNLS. Using cross-reinnervation and self-reinnervation surgery in which motor axons are disconnected from their target muscle and reconnected to a new muscle, we show that FF MNs remain hTDP-43ΔNLS-susceptible and slow MNs remain resistant, regardless of which muscle fibers they control. Collectively, these findings demonstrate that MN identity dictates the susceptibility of neuromuscular junctions to TDP-43 pathology and slow MNs can drive recovery of motor systems due to their remarkable resilience to TDP-43-driven degeneration. This study highlights a potential pathway for regaining motor function with ALS pathology in the advent of therapies that halt the underlying neurodegenerative process.

Published

2022

27. Traumatic brain injury and post-traumatic stress disorder are not associated with Alzheimer's disease pathology measured with biomarkers

Author

Michael W, Weiner, Danielle, Harvey, Susan M, Landau, Dallas P, Veitch, Thomas C, Neylan, Jordan H, Grafman, Paul S, Aisen, Ronald C, Petersen, Clifford R, Jack, Duygu, Tosun, Leslie M, Shaw, John Q, Trojanowski, Andrew J, Saykin, Jacqueline, Hayes, and Charles, De Carli

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Neurology (clinical), Geriatrics and Gerontology

Abstract

Epidemiological studies report an association between traumatic brain injury (TBI) and post-traumatic stress disorder (PTSD) and clinically diagnosed Alzheimer's disease (AD). We examined the association between TBI/PTSD and biomarker-defined AD.We identified 289 non-demented veterans with TBI and/or PTSD and controls who underwent clinical evaluation, cerebrospinal fluid (CSF) collection, magnetic resonance imaging (MRI), amyloid beta (Aβ) and tau positron emission tomography, and apolipoprotein E testing. Participants were followed for up to 5.2 years.Exposure groups (TBI, PTSD, and TBI + PTSD) had higher prevalence of mild cognitive impairment (MCI: P .0001) and worse Mini-Mental State Examination scores (PTSD: P = .008; TBIPTSD: P = .009) than controls. There were no significant differences in other cognitive scores, MRI volumes, Aβ or tau accumulation, or in most longitudinal measures.TBI and/or PTSD were not associated with elevated AD biomarkers. The poorer cognitive status of exposed veterans may be due to other comorbid pathologies.

Published

2022

28. Plasma MIA, CRP, and Albumin Predict Cognitive Decline in Parkinson's Disease

Author

Junchao Shen, Noor Amari, Rebecca Zack, R. Tyler Skrinak, Travis L. Unger, Marijan Posavi, Thomas F. Tropea, Sharon X. Xie, Vivianna M. Van Deerlin, Richard B. Dewey, Daniel Weintraub, John Q. Trojanowski, and Alice S. Chen‐Plotkin

Subjects

Extracellular Matrix Proteins, C-Reactive Protein, Neurology, Albumins, Humans, Cognitive Dysfunction, Dementia, Parkinson Disease, Neurology (clinical), Neuropsychological Tests, Biomarkers, Serum Albumin, Neoplasm Proteins

Abstract

Using a multi-cohort, discovery-replication-validation design, we sought new plasma biomarkers that predict which individuals with Parkinson's disease (PD) will experience cognitive decline.In 108 discovery cohort PD individuals and 83 replication cohort PD individuals, we measured 940 plasma proteins on an aptamer-based platform. Using proteins associated with subsequent cognitive decline in both cohorts, we trained a logistic regression model to predict which patients with PD showed fast ( = 1 point drop/year on Montreal Cognitive Assessment [MoCA]) versus slow ( 1 point drop/year on MoCA) cognitive decline in the discovery cohort, testing it in the replication cohort. We developed alternate assays for the top 3 proteins and confirmed their ability to predict cognitive decline - defined by change in MoCA or development of incident mild cognitive impairment (MCI) or dementia - in a validation cohort of 118 individuals with PD. We investigated the top plasma biomarker for causal influence by Mendelian randomization (MR).A model with only 3 proteins (melanoma inhibitory activity protein [MIA], C-reactive protein [CRP], and albumin) separated fast versus slow cognitive decline subgroups with an area under the curve (AUC) of 0.80 in the validation cohort. The individuals with PD in the validation cohort in the top quartile of risk for cognitive decline based on this model were 4.4 times more likely to develop incident MCI or dementia than those in the lowest quartile. Genotypes at MIA single nucleotide polymorphism (SNP) rs2233154 associated with MIA levels and cognitive decline, providing evidence for MIA's causal influence.An easily obtained plasma-based predictor identifies individuals with PD at risk for cognitive decline. MIA may participate causally in development of cognitive decline. ANN NEUROL 2022;92:255-269.

Published

2022

29. Investigating key factors underlying neurodegeneration linked to alpha-synuclein spread

Author

Cindy C. C. Pang, Maja H. Sørensen, Krit Lee, Kelvin C. Luk, John Q. Trojanowski, Virginia M. Y. Lee, Wendy Noble, and Raymond C. C. Chang

Subjects

Rats, Sprague-Dawley, Substantia Nigra, Mice, Histology, Neurology, Physiology (medical), alpha-Synuclein, Animals, Parkinson Disease, Neurology (clinical), Oxidopamine, Pathology and Forensic Medicine, Rats

Abstract

It has long been considered that accumulation of pathological alpha-synuclein (aSyn) leads to synaptic/neuronal loss which then results in behavioural and cognitive dysfunction. To investigate this claim, we investigated effects downstream of aSyn preformed fibrils (PFFs) and 6-hydroxydopamine (6-OHDA), because aSyn PFFs induce spreading/accumulation of aSyn, and 6-OHDA rapidly causes local neuronal loss.We injected mouse aSyn PFFs into the medial forebrain bundle (MFB) of Sprague-Dawley rats. We investigated spread of pathological aSyn, phosphorylation of aSyn and tau, oxidative stress, synaptic/neuronal loss and cognitive dysfunction 60, 90 and 120 days after injection. Similarly, we injected 6-OHDA into the MFB and examined the same parameters 1 and 3 weeks after injection.Following aSyn PFF injection, phosphorylated aSyn was found distant from the injection site in the hippocampus and frontal cortex. However, despite neuron loss being evident close to the site of injection in the substantia nigra at 120 days post injection, there were no other neurodegeneration-associated features associated with aSyn including synaptic loss. In contrast, 6-OHDA caused severe neuronal loss in the substantia nigra at 3 weeks post injection that was accompanied by phosphorylation of aSyn and tau, oxidative stress, loss of synaptic proteins, cognitive and motor dysfunction.Our results demonstrate that spread/replication and slow accumulation of pathological aSyn may not be sufficient to induce neurodegenerative changes. In contrast, oxidative stress responses in addition to aSyn accumulation were associated with other Parkinson's disease (PD)-associated abnormalities and cognitive dysfunction. Our results may be important when considering why only some PD patients develop dementia.

Published

2022

30. Natural speech markers of Alzheimer's disease co-pathology in Lewy body dementias

Author

Sanjana Shellikeri, Sunghye Cho, Katheryn A.Q. Cousins, Mark Liberman, Erica Howard, Yvonne Balganorth, Daniel Weintraub, Meredith Spindler, Andres Deik, Edward B. Lee, John Q. Trojanowski, David Irwin, David Wolk, Murray Grossman, and Naomi Nevler

Subjects

Lewy Body Disease, Amyloid beta-Peptides, Parkinson Disease, tau Proteins, Article, Neurology, Alzheimer Disease, alpha-Synuclein, Humans, Speech, Dementia, Neurology (clinical), Geriatrics and Gerontology, Biomarkers

Abstract

INTRODUCTION: An estimated 50% of patients with Lewy body dementias (LBD), including Parkinson’s disease dementia (PDD) and Dementia with Lewy bodies (DLB), have co-occurring Alzheimer’s disease (AD) that is associated with worse prognosis. This study tests an automated analysis of natural speech as an inexpensive, non-invasive screening tool for AD co-pathology in biologically-confirmed cohorts of LBD patients with AD co-pathology (SYN + AD) and without (SYN-AD). METHODS: We analyzed lexical-semantic and acoustic features of picture descriptions using automated methods in 22 SYN + AD and 38 SYN-AD patients stratified using AD CSF biomarkers or autopsy diagnosis. Speech markers of AD co-pathology were identified using best subset regression, and their diagnostic discrimination was tested using receiver operating characteristic. ANCOVAs compared measures between groups covarying for demographic differences and cognitive disease severity. We tested relations with CSF tau levels, and compared speech measures between PDD and DLB clinical disorders in the same cohort. RESULTS: Age of acquisition of nouns (p = 0.034, |d| = 0.77) and lexical density (p = 0.0064, |d| = 0.72) were reduced in SYN + AD, and together showed excellent discrimination for SYN + AD vs. SYN-AD (95% sensitivity, 66% specificity; AUC = 0.82). Lower lexical density was related to higher CSF t-Tau levels (R = −0.41, p = 0.0021). Clinically-diagnosed PDD vs. DLB did not differ on any speech features. CONCLUSION: AD co-pathology may result in a deviant natural speech profile in LBD characterized by specific lexical-semantic impairments, not detectable by clinical disorder diagnosis. Our study demonstrates the potential of automated digital speech analytics as a screening tool for underlying AD co-pathology in LBD.

Published

2022

31. Elevated plasma phosphorylated tau 181 in amyotrophic lateral sclerosis relates to lower motor neuron dysfunction

Author

Katheryn A.Q. Cousins, Leslie M. Shaw, Sanjana Shellikeri, Laynie Dratch, Luis Rosario, Lauren B. Elman, Colin Quinn, Defne A. Amado, David A. Wolk, Thomas F. Tropea, Alice Chen-Plotkin, David J. Irwin, Murray Grossman, Edward B. Lee, John Q. Trojanowski, and Corey T. McMillan

Abstract

ObjectivePlasma phosphorylated tau (p-tau181) is reliably elevated in Alzheimer’s disease (AD), but less explored is its specificity relative to other neurodegenerative conditions. Here we find novel evidence that plasma p-tau181 is elevated in amytrophic lateral sclerosis (ALS), a neurodegenerative condition typically lacking tau pathology. We performed a detailed clinical evaluation to unravel the potential source of this unexpected observation.MethodsPatients were clinically or pathologically diagnosed with ALS (n=130) or AD (n=82), or were healthy non-impaired controls (n=33). Receiver operating characteristic (ROC) curves were analyzed and area under the curve (AUC) was used to discriminate AD from ALS. Within ALS, Mann-Whitney-Wilcoxon tests compared analytes by presence/absence of upper motor neuron (UMN) and lower motor neuron (LMN) signs. Spearman correlations tested associations between plasma p-tau181 and postmortem neuron loss.ResultsA Wilcoxon test showed plasma p-tau181 was higher in ALS than controls (W=3297, p=0.0000020), and ROC analyses showed plasma p-tau181 poorly discriminated AD and ALS (AUC=0.60). In ALS, elevated plasma p-tau181 was associated with LMN signs in cervical (W=827, p=0.0072), thoracic (W=469, p=0.00025), and lumbosacral regions (W=851, p=0.0000029). In support of LMN findings, plasma p-tau181 was associated with neuron loss in the spinal cord (rho=0.46, p=0.017), but not in the motor cortex (p=0.41). CSF p-tau181 and plasma neurofilament light chain (NfL) were included as reference analytes, and demonstrate specificity of findings.InterpretationWe found strong evidence that plasma p-tau181 is elevated in ALS and may be a novel marker specific to LMN dysfunction.

Published

2022

32. ApoJ/Clusterin concentrations are determinants of cerebrospinal fluid cholesterol efflux capacity and reduced levels are associated with Alzheimer's disease

Author

Yi-An, Ko, Jeffrey T, Billheimer, Nicholas N, Lyssenko, Alexandra, Kueider-Paisley, David A, Wolk, Steven E, Arnold, Yuk Yee, Leung, Leslie M, Shaw, John Q, Trojanowski, Rima F, Kaddurah-Daouk, Mitchel A, Kling, and Daniel J, Rader

Subjects

Mice, Neuroblastoma, Clusterin, Apolipoproteins E, Cholesterol, Apolipoprotein A-I, Alzheimer Disease, Cardiovascular Diseases, Humans, Animals, Neurodegenerative Diseases

Abstract

Alzheimer's disease (AD) shares risk factors with cardiovascular disease (CVD) and dysregulated cholesterol metabolism is a mechanism common to both diseases. Cholesterol efflux capacity (CEC) is an ex vivo metric of plasma high-density lipoprotein (HDL) function and inversely predicts incident CVD independently of other risk factors. Cholesterol pools in the central nervous system (CNS) are largely separate from those in blood, and CNS cholesterol excess may promote neurodegeneration. CEC of cerebrospinal fluid (CSF) may be a useful measure of CNS cholesterol trafficking. We hypothesized that subjects with AD and mild cognitive impairment (MCI) would have reduced CSF CEC compared with Cognitively Normal (CN) and that CSF apolipoproteins apoA-I, apoJ, and apoE might have associations with CSF CEC.We retrieved CSF and same-day ethylenediaminetetraacetic acid (EDTA) plasma from 108 subjects (40 AD; 18 MCI; and 50 CN) from the Center for Neurodegenerative Disease Research biobank at the Perelman School of Medicine, University of Pennsylvania. For CSF CEC assays, we used N9 mouse microglial cells and SH-SY5Y human neuroblastoma cells, and the corresponding plasma assay used J774 cells. Cells were labeled with [We found that CSF CEC was significantly lower in MCI compared with controls and was poorly correlated with plasma CEC. CSF levels of ApoJ/Clusterin were also significantly lower in MCI and were significantly associated with CSF CEC. While CSF ApoA-I was also associated with CSF CEC, CSF ApoE had no association with CSF CEC. CSF CEC is significantly and positively associated with CSF Aβ. Taken together, ApoJ/Clusterin may be an important determinant of CSF CEC, which in turn could mitigate risk of MCI and AD risk by promoting cellular efflux of cholesterol or other lipids. In contrast, CSF ApoE does not appear to play a role in determining CSF CEC.

Published

2022

33. Plasma MIA, CRP, and albumin predict cognitive decline in Parkinson’s Disease

Author

Junchao Shen, Noor Amari, Rebecca Zack, R. Tyler Skrinak, Travis L. Unger, Marijan Posavi, Thomas F. Tropea, Sharon X. Xie, Vivianna M. Van Deerlin, Richard B. Dewey, Daniel Weintraub, John Q. Trojanowski, and Alice S. Chen-Plotkin

Abstract

ObjectiveUsing a multi-cohort, Discovery-Replication-Validation design, we sought new plasma biomarkers that predict which PD individuals will experience cognitive decline.MethodsIn 108 Discovery Cohort PD individuals and 83 Replication Cohort PD individuals, we measured 940 plasma proteins on an aptamer-based platform. Using proteins associating with subsequent cognitive decline in both cohorts, we trained a logistic regression model to predict which PD patients showed fast (>=1 point drop/year on Montreal Cognitive Assessment (MoCA)) vs. slow (ResultsA model with only three proteins (Melanoma Inhibitory Activity Protein (MIA), C-Reactive Protein (CRP), albumin) separated Fast vs. Slow cognitive decline subgroups with an AUC of 0.80 in the Validation Cohort. Validation Cohort PD individuals in the top quartile of risk for cognitive decline based on this model were 4.4 times more likely to develop incident MCI or dementia than those in the lowest quartile. Genotypes at MIA SNP rs2233154 associated with MIA levels and cognitive decline, providing evidence for MIA’s causal influence.ConclusionsAn easily-obtained plasma-based predictor identifies PD individuals at risk for cognitive decline. MIA may participate causally in development of cognitive decline.

Published

2022

34. TMEM106B deficiency impairs cerebellar myelination and synaptic integrity with Purkinje cell loss

Author

Tuancheng Feng, Lin Luan, Isabel Iscol Katz, Mohammed Ullah, Vivianna M. Van Deerlin, John Q. Trojanowski, Edward B. Lee, and Fenghua Hu

Subjects

Brain Diseases, Mice, Purkinje Cells, Cellular and Molecular Neuroscience, nervous system, Frontotemporal Dementia, Animals, Membrane Proteins, Nerve Tissue Proteins, Neurology (clinical), Frontotemporal Lobar Degeneration, Pathology and Forensic Medicine

Abstract

TMEM106B, a type II lysosomal transmembrane protein, has recently been associated with brain aging, hypomyelinating leukodystrophy, frontotemporal lobar degeneration (FTLD) and several other brain disorders. TMEM106B is critical for proper lysosomal function and TMEM106B deficiency leads to myelination defects, FTLD related pathology, and motor coordination deficits in mice. However, the physiological and pathological functions of TMEM106B in the brain are still not well understood. In this study, we investigate the role of TMEM106B in the cerebellum, dysfunction of which has been associated with FTLD and other brain disorders. We found that TMEM106B is ubiquitously expressed in neurons in the cerebellum, with the highest levels in the Purkinje neurons. Aged TMEM106B-deficient mice show significant loss of Purkinje neurons specifically in the anterior lobe of the cerebellum. Increased microglia and astrocyte activation, as well as an accumulation of ubiquitinated proteins, p62 and TDP-43 were also detected in the cerebellum of aged TMEM106B deficient mice. In the young mice, myelination defects and a significant loss of synapses between Purkinje and deep cerebellar nuclei neurons were observed. Interestingly, TMEM106B deficiency causes distinct lysosomal phenotypes in different types of neurons and glia in the cerebellum and frontal cortex. In humans, TMEM106B rs1990622 risk allele (T/T) is associated with increased Purkinje neuron loss. Taken together, our studies support that TMEM106B regulates lysosomal function in a cell-type-specific manner and TMEM106B is critical for maintaining synaptic integrity and neural functions in the cerebellum.

Published

2022

35. Tau pathology associates with in vivo cortical thinning in Lewy body disorders

Author

James F. Morley, Nabila Dahodwala, Leslie M. Shaw, John E. Duda, John Q. Trojanowski, Murray Grossman, Sanjeev N. Vaishnavi, David G. Coughlin, Corey T. McMillan, Alice Chen-Plotkin, David A. Wolk, Meredith Spindler, David J. Irwin, Christopher Olm, Nicola Spotorno, Daniel Weintraub, Andres Deik, and Edward B. Lee

Subjects

Male, 0301 basic medicine, Aging, Pathology, Neocortex, Autopsy, Comorbidity, Neurodegenerative, Alzheimer's Disease, 0302 clinical medicine, 2.1 Biological and endogenous factors, Aetiology, Alzheimer's Disease Related Dementias (ADRD), Research Articles, Parkinson's Disease, General Neuroscience, Neurodegeneration, Parkinson Disease, Middle Aged, medicine.anatomical_structure, Neurological, Female, hormones, hormone substitutes, and hormone antagonists, Research Article, Lewy Body Disease, medicine.medical_specialty, Lewy Body Dementia, Clinical Sciences, tau Proteins, 03 medical and health sciences, Atrophy, Alzheimer Disease, In vivo, Acquired Cognitive Impairment, medicine, Humans, Dementia, Cognitive Dysfunction, Retrospective Studies, Aged, Lewy body, business.industry, Prevention, Neurosciences, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), medicine.disease, Brain Disorders, 030104 developmental biology, Histopathology, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

ObjectivesTo investigate the impact of Alzheimer's disease (AD) co-pathology on an in vivo structural measure of neurodegeneration in Lewy body disorders (LBD).MethodsWe studied 72 LBD patients (Parkinson disease (PD)=2, PD-MCI=25, PD with dementia=10, dementia with Lewy bodies=35) with either CSF analysis or neuropathological examination and structural MRI during life. The cohort was divided into those harboring significant AD co-pathology, either at autopsy (intermediate/high AD neuropathologic change) or with CSF signature indicating AD co-pathology (t-tau/Aβ1-42 >0.3) (LBD+AD, N=19), and those without AD co-pathology (LBD-AD, N=53). We also included a reference group of 25 patients with CSF biomarker-confirmed amnestic AD. We investigated differences in MRI cortical thickness estimates between groups, and in the 21 autopsied LBD patients (LBD-AD=14, LBD+AD=7), directly tested the association between antemortem MRI and post-mortem burdens of tau, Aβ, and alpha-synuclein using digital histopathology in five representative neocortical regions.ResultsThe LBD+AD group was characterized by cortical thinning in anterior/medial and lateral temporal regions (P&nbsp

Published

2020

36. Discovery and Functional Characterization of hPT3, a Humanized Anti-Phospho Tau Selective Monoclonal Antibody

Author

Thomas J. Malia, Marc Vandermeeren, Hong Sun, Kristof Van Kolen, Marc Mercken, Rupesh Nanjunda, Gallen Triana-Baltzer, M. Borgers, Astrid Bottelbergs, Eilyn R. Lacy, Alexey Teplyakov, Tom Van De Casteele, John Q. Trojanowski, Clara Theunis, Hervé Maurin, Peter Larsen, Robin Ernst, Sheng-Jiun Wu, Cindy Wintmolders, Roland Willems, Randy Slemmon, Wendy Galpern, and Jinquan Luo

Subjects

0301 basic medicine, medicine.drug_class, medicine.medical_treatment, Tau protein, tau Proteins, Antibodies, Monoclonal, Humanized, Monoclonal antibody, Neutralization, Mice, 03 medical and health sciences, 0302 clinical medicine, In vivo, Drug Discovery, medicine, Animals, Humans, Phosphorylation, Mice, Knockout, Mice, Inbred BALB C, biology, Chemistry, General Neuroscience, Antibodies, Monoclonal, General Medicine, Immunotherapy, In vitro, Protein Structure, Tertiary, Psychiatry and Mental health, Clinical Psychology, 030104 developmental biology, Cancer research, biology.protein, Immunohistochemistry, Geriatrics and Gerontology, Antibody, 030217 neurology & neurosurgery

Abstract

Background: As a consequence of the discovery of an extracellular component responsible for the progression of tau pathology, tau immunotherapy is being extensively explored in both preclinical and clinical studies as a disease modifying strategy for the treatment of Alzheimer’s disease. Objective: Describe the characteristics of the anti-phospho (T212/T217) tau selective antibody PT3 and its humanized variant hPT3. Methods: By performing different immunization campaigns, a large collection of antibodies has been generated and prioritized. In depth, in vitro characterization using surface plasmon resonance, phospho-epitope mapping, and X-ray crystallography experiments were performed. Further characterization involved immunohistochemical staining on mouse- and human postmortem tissue and neutralization of tau seeding by immunodepletion assays. Results and Conclusion: Various in vitro experiments demonstrated a high intrinsic affinity for PT3 and hPT3 for AD brain-derived paired helical filaments but also to non-aggregated phospho (T212/T217) tau. Further functional analyses in cellular and in vivo models of tau seeding demonstrated almost complete depletion of tau seeds in an AD brain homogenate. Ongoing trials will provide the clinical evaluation of the tau spreading hypothesis in Alzheimer’s disease.

Published

2020

37. Limbic-predominant age-related TDP-43 encephalopathy differs from frontotemporal lobar degeneration

Author

Panpan Zhang, Peter T. Nelson, John Q. Trojanowski, Sharon X. Xie, EunRan Suh, Sílvia Porta, Justin M. Barber, Gregory A. Jicha, Edward B. Lee, John L. Robinson, Virginia M.-Y. Lee, Filip G. Garrett, Erin L. Abner, and Vivianna M. Van Deerlin

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Encephalopathy, Autopsy, TARDBP, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, C9orf72, Internal medicine, mental disorders, Limbic System, Humans, Medicine, Pathological, Aged, Aged, 80 and over, business.industry, Age Factors, nutritional and metabolic diseases, Original Articles, Frontotemporal lobar degeneration, Middle Aged, medicine.disease, nervous system diseases, 030104 developmental biology, TDP-43 Proteinopathies, Cohort, Female, Neurology (clinical), Frontotemporal Lobar Degeneration, business, 030217 neurology & neurosurgery, Frontotemporal dementia

Abstract

TAR-DNA binding protein-43 (TDP-43) proteinopathy is seen in multiple brain diseases. A standardized terminology was recommended recently for common age-related TDP-43 proteinopathy: limbic-predominant, age-related TDP-43 encephalopathy (LATE) and the underlying neuropathological changes, LATE-NC. LATE-NC may be co-morbid with Alzheimer’s disease neuropathological changes (ADNC). However, there currently are ill-defined diagnostic classification issues among LATE-NC, ADNC, and frontotemporal lobar degeneration with TDP-43 (FTLD-TDP). A practical challenge is that different autopsy cohorts are composed of disparate groups of research volunteers: hospital- and clinic-based cohorts are enriched for FTLD-TDP cases, whereas community-based cohorts have more LATE-NC cases. Neuropathological methods also differ across laboratories. Here, we combined both cases and neuropathologists’ diagnoses from two research centres—University of Pennsylvania and University of Kentucky. The study was designed to compare neuropathological findings between FTLD-TDP and pathologically severe LATE-NC. First, cases were selected from the University of Pennsylvania with pathological diagnoses of either FTLD-TDP (n = 33) or severe LATE-NC (mostly stage 3) with co-morbid ADNC (n = 30). Sections from these University of Pennsylvania cases were cut from amygdala, anterior cingulate, superior/mid-temporal, and middle frontal gyrus. These sections were stained for phospho-TDP-43 immunohistochemically and evaluated independently by two University of Kentucky neuropathologists blinded to case data. A simple set of criteria hypothesized to differentiate FTLD-TDP from LATE-NC was generated based on density of TDP-43 immunoreactive neuronal cytoplasmic inclusions in the neocortical regions. Criteria-based sensitivity and specificity of differentiating severe LATE-NC from FTLD-TDP cases with blind evaluation was ∼90%. Another proposed neuropathological feature related to TDP-43 proteinopathy in aged individuals is ‘Alpha’ versus ‘Beta’ in amygdala. Alpha and Beta status was diagnosed by neuropathologists from both universities (n = 5 raters). There was poor inter-rater reliability of Alpha/Beta classification (mean κ = 0.31). We next tested a separate cohort of cases from University of Kentucky with either FTLD-TDP (n = 8) or with relatively ‘pure’ severe LATE-NC (lacking intermediate or severe ADNC; n = 14). The simple criteria were applied by neuropathologists blinded to the prior diagnoses at University of Pennsylvania. Again, the criteria for differentiating LATE-NC from FTLD-TDP was effective, with sensitivity and specificity ∼90%. If more representative cases from each cohort (including less severe TDP-43 proteinopathy) had been included, the overall accuracy for identifying LATE-NC was estimated at >98% for both cohorts. Also across both cohorts, cases with FTLD-TDP died younger than those with LATE-NC (P

Published

2020

38. Insoluble Tau From Human FTDP-17 Cases Exhibit Unique Transmission Properties In Vivo

Author

Zhuohao He, Bin Zhang, Gerard D. Schellenberg, John Q. Trojanowski, Sneha Narasimhan, Sarah A Weitzman, Virginia M.-Y. Lee, Jennifer D. McBride, and Lakshmi Changolkar

Subjects

Male, Cell, Tau protein, tau Proteins, Neuropathology, Biology, Pathology and Forensic Medicine, Mice, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, mental disorders, medicine, Animals, Humans, Gene, 030304 developmental biology, 0303 health sciences, Original Articles, General Medicine, medicine.disease, Cell biology, Mice, Inbred C57BL, Chromosome 17 (human), medicine.anatomical_structure, Neurology, Frontotemporal Dementia, biology.protein, Female, Neurology (clinical), Tauopathy, 030217 neurology & neurosurgery, Intracellular, Frontotemporal dementia

Abstract

One hallmark of neurodegenerative diseases is the intracellular accumulation of hyperphosphorylated tau protein, a neuronal microtubule-associated protein, into structures known as neurofibrillary tangles. Tauopathies are heterogeneous neurodegenerative diseases caused by the misfolding of the tau protein. It has been previously shown that the tau protein can spread from cell to cell in a prion-like manner. Tauopathies can be sporadic or familial, with the identification of pathogenic mutations in the microtubule-associated protein tau gene on chromosome 17 in the familial cases. Different frontotemporal dementia with parkinsonism-17 (FTDP-17) cases are associated with varying clinical presentations and types of neuropathology. We previously demonstrated that insoluble tau extracted from sporadic tauopathy human brains contain distinct tau strains, which underlie the heterogeneity of these diseases. Furthermore, these tau strains seeded tau aggregates that resemble human tau neuropathology in nontransgenic and 6hTau mice in vivo. Here, we show insoluble tau from human brains of FTDP-17 cases transmit different patterns of neuronal and glial tau pathology in vivo, similar to the sporadic tauopathies. This suggests that each of these tau mutations has unique properties that underlie the heterogeneity of FTDP-17 cases.

Published

2020

39. Evolution of Alzheimer's Disease Cerebrospinal Fluid Biomarkers in Early Parkinson's Disease

Author

Samantha J. Hutten, Douglas Galasko, Ju-Hee Kang, John Q. Trojanowski, Arthur W. Toga, Leslie M. Shaw, Andrew Siderowf, Caroline M. Tanner, Parkinson's Progression Marker Initiative, Daniel Weintraub, Alyssa Reimer, Brit Mollenhauer, David J. Irwin, Janel Fedler, Karl Kieburtz, Christopher S. Coffey, Kenneth Marek, Tanya Simuni, Chelsea Caspell-Garcia, Lana M. Chahine, and Tatiana Foroud

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Parkinson's disease, tau Proteins, Disease, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Cerebrospinal fluid, Alzheimer Disease, Internal medicine, medicine, Humans, Longitudinal Studies, Prospective Studies, Healthy aging, Prospective cohort study, Research Articles, Aged, Amyloid beta-Peptides, business.industry, Parkinson Disease, Middle Aged, medicine.disease, 3. Good health, 030104 developmental biology, Neurology, Csf biomarkers, Disease Progression, Biomarker (medicine), Csf analysis, Female, Neurology (clinical), business, Biomarkers, 030217 neurology & neurosurgery, Research Article

Abstract

Author(s): Irwin, David J; Fedler, Janel; Coffey, Christopher S; Caspell-Garcia, Chelsea; Kang, Ju Hee; Simuni, Tanya; Foroud, Tatiana; Toga, Arthur W; Tanner, Caroline M; Kieburtz, Karl; Chahine, Lana M; Reimer, Alyssa; Hutten, Samantha; Weintraub, Daniel; Mollenhauer, Brit; Galasko, Douglas R; Siderowf, Andrew; Marek, Kenneth; Trojanowski, John Q; Shaw, Leslie M; Parkinson's Progression Marker Initiative | Abstract: ObjectiveWe analyzed the longitudinal profile of Alzheimer's disease (AD) cerebrospinal fluid (CSF) biomarkers in early Parkinson's disease (PD) compared with healthy controls (HCs) and tested baseline CSF biomarkers for prediction of clinical decline in PD.MethodsAmyloid-β 1 to 42 (Aβ42 ), total tau (t-tau) and phosphorylated tau (p-tau) at the threonine 181 position were measured using the high-precision Roche Elecsys electrochemiluminescence immunoassay in all available CSF samples from longitudinally studied patients with PD (n = 416) and HCs (n = 192) followed for up to 3 years in the Parkinson's Progression Markers Initiative (PPMI). Longitudinal CSF and clinical data were analyzed with linear-mixed effects models.ResultsWe found patients with PD had lower CSF t-tau (median = 157.7 pg/mL; range = 80.9-467.0); p-tau (median = 13.4 pg/mL; range = 8.0-40.1), and Aβ42 (median = 846.2 pg/mL; range = 238.8-3,707.0) than HCs at baseline (CSF t-tau median = 173.5 pg/mL; range = 82.0-580.8; p-tau median = 15.4 pg/mL; range = 8.1-73.6; and Aβ42 median = 926.5 pg/mL; range = 239.1-3,297.0; p l 0.05-0.001) and a moderate-to-strong correlation among these biomarkers in both patients with PD and HCs (Rho = 0.50-0.97; p l 0.001). Of the patients with PD, 31.5% had pathologically low levels of CSF Aβ42 at baseline and these patients with PD had lower p-tau levels (median = 10.8 pg/mL; range = 8.0-32.8) compared with 27.7% of HCs with pathologically low CSF Aβ42 (CSF p-tau median = 12.8 pg/mL; range 8.2-73.6; p l 0.03). In longitudinal CSF analysis, we found patients with PD had greater decline in CSF Aβ42 (mean difference = -41.83 pg/mL; p = 0.03) and CSF p-tau (mean difference = -0.38 pg/mL; p = 0.03) at year 3 compared with HCs. Baseline CSF Aβ42 values predicted small but measurable decline on cognitive, autonomic, and motor function in early PD.InterpretationOur data suggest baseline CSF AD biomarkers may have prognostic value in early PD and that the dynamic change of these markers, although modest over a 3-year period, suggest biomarker profiles in PD may deviate from healthy aging. ANN NEUROL 2020;88:574-587.

Published

2020

40. Subjective Cognitive Complaint in Parkinson's Disease Patients With Normal Cognition: Canary in the Coal Mine?

Author

Daniel Weintraub, Benjamin L. Deck, Jacqueline Rick, John E. Duda, Sharon X. Xie, Andrew Siderowf, Rachael Purri, Alice Chen-Plotkin, John Q. Trojanowski, Rizwan S. Akhtar, Nabila Dahodwala, Lana M. Chahine, Laura Brennan, and James F. Morley

Subjects

0301 basic medicine, medicine.medical_specialty, Parkinson's disease, Trail Making Test, Neuropsychological Tests, Audiology, Article, 03 medical and health sciences, Cognition, 0302 clinical medicine, medicine, Humans, Dementia, Cognitive Dysfunction, Functional ability, Cognitive decline, business.industry, Hazard ratio, Parkinson Disease, medicine.disease, Cognitive test, Coal, 030104 developmental biology, Neurology, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

Objective The objective of this study was to determine the frequency and impact of subjective cognitive complaint (SCC) in Parkinson's disease (PD) patients with normal cognition. Methods Patients with PD with expert consensus-determined normal cognition at baseline were asked a single question regarding the presence of SCC. Baseline (N = 153) and longitudinal (up to 4 follow-up visits during a 5-year period; N = 121) between-group differences in patients with PD with (+SCC) and without (-SCC) cognitive complaint were examined, including cognitive test performance and self-rated and informant-rated functional abilities. Results A total of 81 (53%) participants reported a cognitive complaint. There were no between-group differences in global cognition at baseline. Longitudinally, the +SCC group declined more than the -SCC group on global cognition (Mattis Dementia Rating Scale-2 total score, F1,431 = 5.71, P = 0.02), processing speed (Symbol Digit Modalities Test, F1,425 = 7.52, P = 0.006), and executive function (Trail Making Test Part B, F1,419 = 4.48, P = 0.04), although the results were not significant after correction for multiple testing. In addition, the +SCC group was more likely to progress to a diagnosis of cognitive impairment over time (hazard ratio = 2.61, P = 0.02). The +SCC group also demonstrated significantly lower self-reported and knowledgeable informant-reported cognition-related functional abilities at baseline, and declined more on an assessment of global functional abilities longitudinally. Conclusions Patients with PD with normal cognition, but with SCC, report poorer cognition-specific functional abilities, and are more likely to be diagnosed with cognitive impairment and experience global functional ability decline long term. These findings suggest that SCC and worse cognition-related functional abilities may be sensitive indicators of initial cognitive decline in PD. © 2020 International Parkinson and Movement Disorder Society.

Published

2020

41. Serum triglycerides in Alzheimer disease

Author

Dinesh Kumar Barupal, Rebecca Baillie, Andrew J. Saykin, Leslie M. Shaw, Tanner Y. Jacobson, Matthias Arnold, P. Murali Doraiswamy, Shannon L. Risacher, Kwangsik Nho, Rima Kaddurah-Daouk, Oliver Fiehn, Megan M. Bernath, Sudeepa Bhattacharyya, Michael W. Weiner, and John Q. Trojanowski

Subjects

Male, 0301 basic medicine, Oncology, medicine.medical_specialty, Amyloid, Neuroimaging, Disease, Neuropsychological Tests, Hippocampus, Article, 03 medical and health sciences, chemistry.chemical_compound, symbols.namesake, Cognition, 0302 clinical medicine, Alzheimer Disease, Internal medicine, medicine, Humans, Cognitive Dysfunction, Triglycerides, Aged, Aged, 80 and over, Amyloid beta-Peptides, Triglyceride, business.industry, Neurodegeneration, medicine.disease, Magnetic Resonance Imaging, 030104 developmental biology, Bonferroni correction, chemistry, Cohort, Disease Progression, symbols, Female, Neurology (clinical), Alzheimer's disease, business, Biomarkers, 030217 neurology & neurosurgery

Abstract

ObjectiveTo investigate the association of triglyceride (TG) principal component scores with Alzheimer disease (AD) and the amyloid, tau, neurodegeneration, and cerebrovascular disease (A/T/N/V) biomarkers for AD.MethodsSerum levels of 84 TG species were measured with untargeted lipid profiling of 689 participants from the Alzheimer's Disease Neuroimaging Initiative cohort, including 190 cognitively normal older adults (CN), 339 with mild cognitive impairment (MCI), and 160 with AD. Principal component analysis with factor rotation was used for dimension reduction of TG species. Differences in principal components between diagnostic groups and associations between principal components and AD biomarkers (including CSF, MRI and [18F]fluorodeoxyglucose-PET) were assessed with a generalized linear model approach. In both cases, the Bonferroni method of adjustment was used to correct for multiple comparisons.ResultsThe 84 TGs yielded 9 principal components, 2 of which, consisting of long-chain, polyunsaturated fatty acid–containing TGs (PUTGs), were significantly associated with MCI and AD. Lower levels of PUTGs were observed in MCI and AD compared to CN. PUTG principal component scores were also significantly associated with hippocampal volume and entorhinal cortical thickness. In participants carrying the APOE ε4 allele, these principal components were significantly associated with CSF β-amyloid1–42 values and entorhinal cortical thickness.ConclusionThis study shows that PUTG component scores were significantly associated with diagnostic group and AD biomarkers, a finding that was more pronounced in APOE ε4 carriers. Replication in independent larger studies and longitudinal follow-up are warranted.

Published

2020

42. Compound screening in cell-based models of tau inclusion formation: Comparison of primary neuron and HEK293 cell assays

Author

Diederik Moechars, Virginia M.-Y. Lee, Charlotte Delay, Anton Simeonov, Kurt R. Brunden, Steve Titus, Mark J. Henderson, John Q. Trojanowski, Alex Crowe, Alexey V. Zakharov, Arjan Buist, and Johnathon Anderson

Subjects

0301 basic medicine, Cell, Tau protein, tau Proteins, Biochemistry, Small Molecule Libraries, Mice, Protein Aggregates, 03 medical and health sciences, Neurobiology, Alzheimer Disease, mental disorders, medicine, Animals, Humans, Senile plaques, Molecular Biology, Neurons, 030102 biochemistry & molecular biology, biology, Chemistry, Neurodegeneration, HEK 293 cells, Neurotoxicity, Cell Biology, medicine.disease, Rats, Dopamine D2 Receptor Antagonists, HEK293 Cells, 030104 developmental biology, medicine.anatomical_structure, Microscopy, Fluorescence, Cancer research, biology.protein, Neuron, Alzheimer's disease

Abstract

The hallmark pathological features of Alzheimer's disease (AD) brains are senile plaques, comprising β-amyloid (Aβ) peptides, and neuronal inclusions formed from tau protein. These plaques form 10–20 years before AD symptom onset, whereas robust tau pathology is more closely associated with symptoms and correlates with cognitive status. This temporal sequence of AD pathology development, coupled with repeated clinical failures of Aβ-directed drugs, suggests that molecules that reduce tau inclusions have therapeutic potential. Few tau-directed drugs are presently in clinical testing, in part because of the difficulty in identifying molecules that reduce tau inclusions. We describe here two cell-based assays of tau inclusion formation that we employed to screen for compounds that inhibit tau pathology: a HEK293 cell-based tau overexpression assay, and a primary rat cortical neuron assay with physiological tau expression. Screening a collection of ∼3500 pharmaceutical compounds with the HEK293 cell tau aggregation assay, we obtained only a low number of hit compounds. Moreover, these compounds generally failed to inhibit tau inclusion formation in the cortical neuron assay. We then screened the Prestwick library of mostly approved drugs in the cortical neuron assay, leading to the identification of a greater number of tau inclusion inhibitors. These included four dopamine D2 receptor antagonists, with D2 receptors having previously been suggested to regulate tau inclusions in a Caenorhabditis elegans model. These results suggest that neurons, the cells most affected by tau pathology in AD, are very suitable for screening for tau inclusion inhibitors.

Published

2020

43. Analytical and Clinical Performance of Amyloid-Beta Peptides Measurements in CSF of ADNIGO/2 Participants by an LC–MS/MS Reference Method

Author

Leslie M. Shaw, Magdalena Brylska, Michal J. Figurski, William J. Jagust, Magdalena Korecka, Jacob Alexander, Susan M. Landau, John Q. Trojanowski, Henrik Zetterberg, and Kaj Blennow

Subjects

0301 basic medicine, Amyloid beta, Concordance, Clinical Biochemistry, Plaque, Amyloid, 03 medical and health sciences, 0302 clinical medicine, Cerebrospinal fluid, Alzheimer Disease, Tandem Mass Spectrometry, Lc ms ms, Humans, Medicine, Cognitive Dysfunction, Amyloid beta-Peptides, Aniline Compounds, medicine.diagnostic_test, biology, business.industry, Amyloidosis, Biochemistry (medical), Clinical performance, Reproducibility of Results, Articles, Reference Standards, medicine.disease, Peptide Fragments, 030104 developmental biology, Certified reference materials, Positron emission tomography, Case-Control Studies, Positron-Emission Tomography, Calibration, biology.protein, Ethylene Glycols, business, Nuclear medicine, Biomarkers, 030217 neurology & neurosurgery, Chromatography, Liquid

Abstract

Background Cerebrospinal fluid (CSF) amyloid-β1-42 (Aβ42) reliably detects brain amyloidosis based on its high concordance with plaque burden at autopsy and with amyloid positron emission tomography (PET) ligand retention observed in several studies. Low CSF Aβ42 concentrations in normal aging and dementia are associated with the presence of fibrillary Aβ across brain regions detected by amyloid PET imaging. Methods An LC–MS/MS reference method for Aβ42, modified by adding Aβ40 and Aβ38 peptides to calibrators, was used to analyze 1445 CSF samples from ADNIGO/2 participants. Seventy runs were completed using 2 different lots of calibrators. For preparation of Aβ42 calibrators and controls spiking solution, reference Aβ42 standard with certified concentration was obtained from EC-JRC-IRMM (Belgium). Aβ40 and Aβ38 standards were purchased from rPeptide. Aβ42 calibrators’ accuracy was established using CSF-based Aβ42 Certified Reference Materials (CRM). Results CRM-adjusted Aβ42 calibrator concentrations were calculated using the regression equation Y (CRM-adjusted) = 0.89X (calibrators) + 32.6. Control samples and CSF pools yielded imprecision ranging from 6.5 to 10.2% (Aβ42) and 2.2 to 7.0% (Aβ40). None of the CSF pools showed statistically significant differences in Aβ42 concentrations across 2 different calibrator lots. Comparison of Aβ42 with Aβ42/Aβ40 showed that the ratio improved concordance with concurrent [18F]-florbetapir PET as a measure of fibrillar Aβ (n = 766) from 81 to 88%. Conclusions Long-term performance assessment substantiates our modified LC–MS/MS reference method for 3 Aβ peptides. The improved diagnostic performance of the CSF ratio Aβ42/Aβ40 suggests that Aβ42 and Aβ40 should be measured together and supports the need for an Aβ40 CRM.

Published

2020

44. Inhibition of CK2 mitigates Alzheimer's tau pathology by preventing NR2B synaptic mislocalization

Author

Courtney A. Marshall, Jennifer D. McBride, Lakshmi Changolkar, Dawn M. Riddle, John Q. Trojanowski, and Virginia M.-Y. Lee

Subjects

Cellular and Molecular Neuroscience, nervous system, Pick Disease of the Brain, Tauopathies, Alzheimer Disease, musculoskeletal, neural, and ocular physiology, Humans, tau Proteins, Neurology (clinical), Casein Kinase II, Receptors, N-Methyl-D-Aspartate, psychological phenomena and processes, Pathology and Forensic Medicine

Abstract

Alzheimer’s disease (AD) is a neurodegenerative disorder that exhibits pathological changes in both tau and synaptic function. AD patients display increases in hyperphosphorylated tau and synaptic activity. Previous studies have individually identified the role of NR2B subunit-containing NMDA receptors in AD related synaptic dysfunction and aggregated tau without reconciling the conflicting differences and implications of NR2B expression. Inhibition of extrasynaptically located NR2B mitigates tau pathology in AD models, whereas the inhibition of synaptic NR2B replicates tau-associated hyperactivity. This suggests that a simultaneous increase in extrasynaptic NR2B and decrease in synaptic NR2B may be responsible for tau pathology and synaptic dysfunction, respectively. The synaptic location of NR2B is regulated by casein kinase 2 (CK2), which is highly expressed in AD patients. Here, we used patient brains diagnosed with AD, corticobasal degeneration, progressive supranuclear palsy or Pick’s disease to characterize CK2 expression across these diverse tauopathies. Human derived material was also utilized in conjunction with cultured hippocampal neurons in order to investigate AD-induced changes in NR2B location. We further assessed the therapeutic effect of CK2 inhibition on NR2B synaptic distribution and tau pathology. We found that aberrant expression of CK2, and synaptically translocated NR2B, is unique to AD patients compared to other tauopathies. Increased CK2 was also observed in AD-tau treated neurons in addition to the mislocalization of NR2B receptors. Tau burden was alleviated in vitro by correcting synaptic:extrasynaptic NR2B function. Restoring NR2B physiological expression patterns with CK2 inhibition and inhibiting the function of excessive extrasynaptic NR2B with Memantine both mitigated tau accumulation in vitro. However, the combined pharmacological treatment promoted the aggregation of tau. Our data suggests that the synaptic:extrasynaptic balance of NR2B function regulates AD-tau pathogenesis, and that the inhibition of CK2, and concomitant prevention of NR2B mislocalization, may be a useful therapeutic tool for AD patients.

Published

2022

45. Tau interactome maps synaptic and mitochondrial processes associated with neurodegeneration

Author

Tara E. Tracy, Jesus Madero-Pérez, Danielle L. Swaney, Timothy S. Chang, Michelle Moritz, Csaba Konrad, Michael E. Ward, Erica Stevenson, Ruth Hüttenhain, Grant Kauwe, Maria Mercedes, Lauren Sweetland-Martin, Xu Chen, Sue-Ann Mok, Man Ying Wong, Maria Telpoukhovskaia, Sang-Won Min, Chao Wang, Peter Dongmin Sohn, Jordie Martin, Yungui Zhou, Wenjie Luo, John Q. Trojanowski, Virginia M.Y. Lee, Shiaoching Gong, Giovanni Manfredi, Giovanni Coppola, Nevan J. Krogan, Daniel H. Geschwind, and Li Gan

Subjects

Proteomics, Aging, interactome, Neurodegenerative, Alzheimer's Disease, Severity of Illness Index, Medical and Health Sciences, protein-protein interaction, synapse, 2.1 Biological and endogenous factors, Protein Interaction Maps, Amino Acids, APEX, Aetiology, Alzheimer's Disease Related Dementias (ADRD), Neurons, Stem Cell Research - Induced Pluripotent Stem Cell - Human, neurodegeneration, Brain, Biological Sciences, Mitochondria, Frontotemporal Dementia (FTD), Tauopathies, Frontotemporal Dementia, Neurological, Disease Progression, Tau secretion, Subcellular Fractions, Protein Binding, Induced Pluripotent Stem Cells, tau Proteins, General Biochemistry, Genetics and Molecular Biology, Protein Domains, Alzheimer Disease, Acquired Cognitive Impairment, Humans, Biotinylation, Cell Nucleus, Stem Cell Research - Induced Pluripotent Stem Cell, affinity purification mass spectrometry, Neurosciences, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Stem Cell Research, Brain Disorders, Synapses, Nerve Degeneration, Mutation, Mutant Proteins, Dementia, Tau, Energy Metabolism, Developmental Biology

Abstract

Tau (MAPT) drives neuronal dysfunction in Alzheimer disease (AD) and other tauopathies. To dissect the underlying mechanisms, we combined an engineered ascorbic acid peroxidase (APEX) approach with quantitative affinity purification mass spectrometry (AP-MS) followed by proximity ligation assay (PLA) to characterize Tau interactomes modified by neuronal activity and mutations that cause frontotemporal dementia (FTD) in human induced pluripotent stem cell (iPSC)-derived neurons. We established interactions of Tau with presynaptic vesicle proteins during activity-dependent Tau secretion and mapped the Tau-binding sites to the cytosolic domains of integral synaptic vesicle proteins. We showed that FTD mutations impair bioenergetics and markedly diminished Tau's interaction with mitochondria proteins, which were downregulated inAD brains of multiple cohorts and correlated with disease severity. These multimodal and dynamic Tau interactomes with exquisite spatial resolution shed light on Tau's role in neuronal function and disease and highlight potential therapeutic targets to block Tau-mediated pathogenesis.

Published

2022

46. Validation of Plasma Amyloid-β 42/40 for Detecting Alzheimer Disease Amyloid Plaques

Author

Yan Li, Suzanne E. Schindler, James G. Bollinger, Vitaliy Ovod, Kwasi G. Mawuenyega, Michael W. Weiner, Leslie M. Shaw, Colin L. Masters, Christopher J. Fowler, John Q. Trojanowski, Magdalena Korecka, Ralph N. Martins, Shorena Janelidze, Oskar Hansson, and Randall J. Bateman

Subjects

Amyloid, Aging, Amyloid beta-Peptides, Neurology & Neurosurgery, Clinical Sciences, Neurosciences, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Plaque, Amyloid, Neurodegenerative, Alzheimer's Disease, Peptide Fragments, Brain Disorders, Good Health and Well Being, Alzheimer Disease, Clinical Research, Positron-Emission Tomography, Neurological, Acquired Cognitive Impairment, Humans, Dementia, Cognitive Sciences, Neurology (clinical), Biomarkers, Research Article, Plaque

Abstract

Background and ObjectivesTo determine the diagnostic accuracy of a plasma Aβ42/Aβ40 assay in classifying amyloid PET status across global research studies using samples collected by multiple centers that utilize different blood collection and processing protocols.MethodsPlasma samples (n = 465) were obtained from 3 large Alzheimer disease (AD) research cohorts in the United States (n = 182), Australia (n = 183), and Sweden (n = 100). Plasma Aβ42/Aβ40 was measured by a high precision immunoprecipitation mass spectrometry (IPMS) assay and compared to the reference standards of amyloid PET and CSF Aβ42/Aβ40.ResultsIn the combined cohort of 465 participants, plasma Aβ42/Aβ40 had good concordance with amyloid PET status (receiver operating characteristic area under the curve [AUC] 0.84, 95% confidence interval [CI] 0.80–0.87); concordance improved with the inclusion of APOE ε4 carrier status (AUC 0.88, 95% CI 0.85–0.91). The AUC of plasma Aβ42/Aβ40 with CSF amyloid status was 0.85 (95% CI 0.78–0.91) and improved to 0.93 (95% CI 0.89–0.97) with APOE ε4 status. These findings were consistent across the 3 cohorts, despite differences in protocols. The assay performed similarly in both cognitively unimpaired and impaired individuals.DiscussionPlasma Aβ42/Aβ40 is a robust measure for detecting amyloid plaques and can be utilized to aid in the diagnosis of AD, identify those at risk for future dementia due to AD, and improve the diversity of populations enrolled in AD research and clinical trials.Classification of EvidenceThis study provides Class II evidence that plasma Aβ42/Aβ40, as measured by a high precision IPMS assay, accurately diagnoses brain amyloidosis in both cognitively unimpaired and impaired research participants.

Published

2022

47. Lateralized

Author

David G, Coughlin, H Branch, Coslett, Claire, Peterson, Jeffrey S, Phillips, Corey, McMillan, Edward B, Lee, John Q, Trojanowski, Murray, Grossman, and David J, Irwin

Abstract

Lewy body diseases are pathologically characterized by α-synuclein pathology. Alzheimer's disease (AD) co-pathology can influence phenotypes. In vivo AD biomarkers can suggest the presence of this co-pathology in unusual cases, but pathological validation remains essential.This patient originally presented with corticobasal syndrome and later developed visual hallucinations and parkinsonism consistent with a synucleinopathy. The patient underwent CSF sampling, 18F-flortaucipir PET scanning, and brain donation with bilateral regions available for digital histological analysis.CSF Aβ42 and t-tau were in the AD range. 18F-flortaucipir scanning showed right-lateralized retention in all lobes (t = 4.3-10.0,This case with overlapping tauopathy and synucleinopathy clinical features had in-depth biomarker characterization and rare bilateral post-mortem sampling showing lateralized tau and α-synuclein pathology suggesting possible synergistic relationships.

Published

2022

48. Lateralized ante mortem and post mortem pathology in a case of Lewy body disease with corticobasal syndrome

Author

David G. Coughlin, H. Branch Coslett, Claire Peterson, Jeffrey S. Phillips, Corey McMillan, Edward B. Lee, John Q. Trojanowski, Murray Grossman, and David J. Irwin

Subjects

Psychiatry and Mental health, Neurology (clinical)

Published

2022

49. Plasma Phosphorylated Tau181 is a Biomarker of Alzheimer's Disease Pathology and Associated with Cognitive and Functional Decline

Author

Thomas F. Tropea, Teresa Waligorska, Sharon X. Xie, Ilya M. Nasralah, Katheryn AQ Cousins, John Q. Trojanowski, Murray Grossman, David J. Irwin, Daniel Weintraub, Edward B. Lee, David A. Wolk, Alice S. Chen-Plotkin, and Leslie M. Shaw

Subjects

History, Polymers and Plastics, Business and International Management, Industrial and Manufacturing Engineering

Published

2022

50. Event-based modeling of T1-weighted MRI is related to pathology in frontotemporal lobar degeneration due to tau and TDP

Author

Christopher A, Olm, Sarah E, Burke, Claire, Peterson, Edward B, Lee, John Q, Trojanowski, Lauren, Massimo, David J, Irwin, Murray, Grossman, and James C, Gee

Subjects

Neurology, Cognitive Neuroscience, Radiology, Nuclear Medicine and imaging, Neurology (clinical)

Abstract

In previous studies of patients with frontotemporal lobar degeneration due to tau (FTLD-tau) and FTLD due to TDP (FTLD-TDP), cortical volumes derived from T1-weighted MRI have been used to identify a sequence of volume loss according to arbitrary volumetric criteria. Event-based modeling (EBM) is a probabilistic, generative machine learning model that determines the characteristic sequence of changes, or "events", occurring during disease progression. EBM also estimates an individual patient's disease "stage" by identifying which events have already occurred. In the present study, we use an EBM analysis to derive stages of regional anatomic atrophy in FTLD-tau and FTLD-TDP, and validated these stages against pathologic burden.Sporadic autopsy-confirmed patients with FTLD-tau (N = 42) and FTLD-TDP (N = 21), and 167 healthy controls with available T1-weighted images were identified. A subset of patients had quantitative digital histopathology of cortex performed at autopsy (FTLD-tau = 30, FTLD-TDP = 17). MRI images were processed, producing regional measures of cortical volumes. K-means clustering was used to find cortical regions with similar amounts of GM volume changes (n = 5 clusters). EBM was used to determine the characteristic sequence of cortical atrophy of identified clusters in autopsy-confirmed FTLD-tau and FTLD-TDP, and estimate each patient's disease stage by cortical volume biomarkers. Linear regressions related pathologic burden to EBM-estimated disease stages.EBM for cortical volume biomarkers generated statistically robust characteristic sequences of cortical atrophy in each group of patients. Cortical volume-based EBM-estimated disease stage was associated with pathologic burden in FTLD-tau (R2 = 0.16, p = 0.017) and FTLD-TDP (R2 = 0.51, p = 0.0008).We provide evidence that EBM can identify sequences of pathologically-confirmed cortical atrophy in sporadic FTLD-tau and FTLD-TDP.

Published

2023