Your search keyword '"Villemagne, Victor L."' showing total 541 results

1. Multimodal neuroimaging biomarkers and subtle cognitive decline in a population-based cohort without dementia.

Author

Weinstein, Andrea M, Fang, Fang, Chang, Chung-Chou H, Cohen, Ann, Lopresti, Brian J, Laymon, Charles M, Nadkarni, Neelesh K, Aizenstein, Howard J, Villemagne, Victor L, Ilyas Kamboh, M, Elizabeth Shaaban, C, Gogniat, Marissa A, Wu, Minjie, Karikari, Thomas K, Ganguli, Mary, and Snitz, Beth E

Subjects

MAGNETIC resonance imaging, ALZHEIMER'S disease, EXECUTIVE function, COGNITION disorders, NEUROPSYCHOLOGICAL tests

Abstract

Background: The relationship between subtle cognitive decline and Alzheimer's disease (AD) pathology as measured by biomarkers in settings outside of specialty memory clinics is not well characterized. Objective: To investigate how subtle longitudinal cognitive decline relates to neuroimaging biomarkers in individuals drawn from a population-based study in an economically depressed, small-town area in southwestern Pennsylvania, USA. Methods: A subset of participants without dementia (N = 115, age 76.53 years ± 6.25) from the Monongahela Youghiogheny Healthy Aging Team (MYHAT) study completed neuroimaging including magnetic resonance imaging (MRI) measures of AD-signature region cortical thickness and white matter hyperintensities (WMH), Pittsburgh compound B (PiB)-positron emission tomography (PET) for amyloid-β (Aβ) deposition, and [18F]AV-1451-PET for tau deposition. Neuropsychological evaluations were completed at multiple timepoints up to 11 years prior to neuroimaging. Aβ positivity was determined using a regional approach. We used linear mixed models to examine neuroimaging biomarker associations with retrospective cognitive slopes in five domains and a global cognitive composite. Results: Among Aβ(+) participants (38%), there were associations between (i) tau Braak III/IV and language decline (p < 0.05), (ii) cortical thickness and both memory decline (p < 0.001) and global cognitive decline (p < 0.01), and (iii) WMH and decline in executive function (p < 0.05) and global cognition (p < 0.05). Among Aβ(-) participants, there was an association between tau Braak III/IV and decline on tests of attention/psychomotor speed (p < 0.05). Conclusions: These findings confirm an Aβ-dependent early AD biomarker pathway, and suggest a possible Aβ-independent, non-AD process underlying subtle cognitive decline in a population-based sample of older adults without dementia. [ABSTRACT FROM AUTHOR]

Published

2025

2. Harmonization of data from neuropsychological tests used in different prospective studies‐ Descending a Tower of Babel.

Author

Shishegar, Rosita, Cox, Timothy, Markovic, Shaun J, Tallapragada, Bhargav, Bourgeat, Pierrick, Dore, Vincent, Laws, Simon M, Porter, Tenielle, Burnham, Samantha C., Feizpour, Azadeh, Weiner, Michael S. W., Hassenstab, Jason J., Morris, John C., Rowe, Christopher C., Villemagne, Victor L, Masters, Colin L., Fripp, Jurgen, Lim, Yen Ying, Doecke, James D., and Sohrabi, Hamid R.

Published

2024

3. Kinetic modeling of the monoamine oxidase-B radioligand [ 18 F]SMBT-1 in human brain with positron emission tomography.

Author

Lopresti, Brian J, Stehouwer, Jeffrey, Reese, Alexandria C, Mason, Neale S, Royse, Sarah K, Narendran, Rajesh, Laymon, Charles M, Lopez, Oscar L, Cohen, Ann D, Mathis, Chester A, and Villemagne, Victor L

Abstract

This paper describes pharmacokinetic analyses of the monoamine-oxidase-B (MAO-B) radiotracer [18F](S)-(2-methylpyrid-5-yl)-6-[(3-fluoro-2-hydroxy)propoxy]quinoline ([18F]SMBT-1) for positron emission tomography (PET) brain imaging. Brain MAO-B expression is widespread, predominantly within astrocytes. Reactive astrogliosis in response to neurodegenerative disease pathology is associated with MAO-B overexpression. Fourteen elderly subjects (8 control, 5 mild cognitive impairment, 1 Alzheimer's disease) with amyloid ([11C]PiB) and tau ([18F]flortaucipir) imaging assessments underwent dynamic [18F]SMBT-1 PET imaging with arterial input function determination. [18F]SMBT-1 showed high brain uptake and a retention pattern consistent with the known MAO-B distribution. A two-tissue compartment (2TC) model where the K1/k2 ratio was fixed to a whole brain value best described [18F]SMBT-1 kinetics. The 2TC total volume of distribution (VT) was well identified and highly correlated (r2∼0.8) with post-mortem MAO-B indices. Cerebellar grey matter (CGM) showed the lowest mean VT of any region and is considered the optimal pseudo-reference region. Simplified analysis methods including reference tissue models, non-compartmental models, and standard uptake value ratios (SUVR) agreed with 2TC outcomes (r2 > 0.9) but with varying bias. We found the CGM-normalized 70–90 min SUVR to be highly correlated (r2 = 0.93) with the 2TC distribution volume ratio (DVR) with acceptable bias (∼10%), representing a practical alternative for [18F]SMBT-1 analyses. [ABSTRACT FROM AUTHOR]

Published

2024

4. Multi-analyte proteomic analysis identifies blood-based neuroinflammation, cerebrovascular and synaptic biomarkers in preclinical Alzheimer's disease.

Author

Zeng, Xuemei, Lafferty, Tara K., Sehrawat, Anuradha, Chen, Yijun, Ferreira, Pamela C. L., Bellaver, Bruna, Povala, Guilherme, Kamboh, M. Ilyas, Klunk, William E., Cohen, Ann D., Lopez, Oscar L., Ikonomovic, Milos D., Pascoal, Tharick A., Ganguli, Mary, Villemagne, Victor L., Snitz, Beth E., and Karikari, Thomas K.

Subjects

ALZHEIMER'S disease, SINGLE molecules, DISEASE progression, CEREBROSPINAL fluid, NUCLEOTIDE sequencing, NEUROFIBRILLARY tangles

Abstract

Background: Blood-based biomarkers are gaining grounds for the detection of Alzheimer's disease (AD) and related disorders (ADRDs). However, two key obstacles remain: the lack of methods for multi-analyte assessments and the need for biomarkers for related pathophysiological processes like neuroinflammation, vascular, and synaptic dysfunction. A novel proteomic method for pre-selected analytes, based on proximity extension technology, was recently introduced. Referred to as the NULISAseq CNS disease panel, the assay simultaneously measures ~ 120 analytes related to neurodegenerative diseases, including those linked to both core (i.e., tau and amyloid-beta (Aβ)) and non-core AD processes. This study aimed to evaluate the technical and clinical performance of this novel targeted proteomic panel. Methods: The NULISAseq CNS disease panel was applied to 176 plasma samples from 113 individuals in the MYHAT-NI cohort of predominantly cognitively normal participants from an economically underserved region in southwestern Pennsylvania, USA. Classical AD biomarkers, including p-tau181, p-tau217, p-tau231, GFAP, NEFL, Aβ40, and Aβ42, were independently measured using Single Molecule Array (Simoa) and correlations and diagnostic performances compared. Aβ pathology, tau pathology, and neurodegeneration (AT(N) statuses) were evaluated with [11C] PiB PET, [18F]AV-1451 PET, and an MRI-based AD-signature composite cortical thickness index, respectively. Linear mixed models were used to examine cross-sectional and Wilcoxon rank sum tests for longitudinal associations between NULISA and neuroimaging-determined AT(N) biomarkers. Results: NULISA concurrently measured 116 plasma biomarkers with good technical performance (97.2 ± 13.9% targets gave signals above assay limits of detection), and significant correlation with Simoa assays for the classical biomarkers. Cross-sectionally, p-tau217 was the top hit to identify Aβ pathology, with age, sex, and APOE genotype-adjusted AUC of 0.930 (95%CI: 0.878–0.983). Fourteen markers were significantly decreased in Aβ-PET + participants, including TIMP3, BDNF, MDH1, and several cytokines. Longitudinally, FGF2, IL4, and IL9 exhibited Aβ PET-dependent yearly increases in Aβ-PET + participants. Novel plasma biomarkers with tau PET-dependent longitudinal changes included proteins associated with neuroinflammation, synaptic function, and cerebrovascular integrity, such as CHIT1, CHI3L1, NPTX1, PGF, PDGFRB, and VEGFA; all previously linked to AD but only reliable when measured in cerebrospinal fluid. The autophagosome cargo protein SQSTM1 exhibited significant association with neurodegeneration after adjusting age, sex, and APOE ε4 genotype. Conclusions: Together, our results demonstrate the feasibility and potential of immunoassay-based multiplexing to provide a comprehensive view of AD-associated proteomic changes, consistent with the recently revised biological and diagnostic framework. Further validation of the identified inflammation, synaptic, and vascular markers will be important for establishing disease state markers in asymptomatic AD. [ABSTRACT FROM AUTHOR]

Published

2024

5. The ADNI PET Core at 20.

Author

Jagust, William J., Koeppe, Robert A., Rabinovici, Gil D., Villemagne, Victor L., Harrison, Theresa M., and Landau, Susan M.

Published

2024

6. Effect of blood collection tube containing protease inhibitors on the pre‐analytical stability of Alzheimer's disease plasma biomarkers.

Author

Chen, Yijun, Zeng, Xuemei, Diaz, Jihui L., Sehrawat, Anuradha, Lafferty, Tara K., Boslett, James J., Klunk, William E., Pascoal, Tharick A., Villemagne, Victor L., Cohen, Ann D., Lopez, Oscar I., Yates, Nathan A., and Karikari, Thomas K.

Subjects

ALZHEIMER'S disease, BLOOD collection, PLASMA stability, BLOOD testing, PROCESS capability

Abstract

The reliability of plasma biomarkers of Alzheimer's disease (AD) can be compromised by protease‐induced degradation. This can limit the feasibility of conducting plasma biomarker studies in environments that lack the capacity for immediate processing and appropriate storage of blood samples. We hypothesized that blood collection tube supplementation with protease inhibitors can improve the stability of plasma biomarkers at room temperatures (RT). In this study, we conducted a comparative analysis of blood biomarker stability in traditional ethylenediaminetetraacetic acid (EDTA) tubes versus BD™ P100 collection tubes, the latter being coated with a protease inhibitor cocktail. The stability of six plasma AD biomarkers was evaluated over time under RT conditions. We evaluated three experimental approaches. In Approach 1, pooled plasma samples underwent storage at RT for up to 96 h. In Approach 2, plasma samples isolated upfront from whole blood collected into EDTA or P100 tubes were stored at RT for 0 h or 24 h before biomarker measurements. In Approach 3, whole blood samples were collected into paired EDTA and P100 tubes, followed by storage at RT for 0 h or 24 h before isolating the plasma for analyses. Biomarkers were measured with Single Molecule Array (Simoa) and immunoprecipitation‐mass spectrometry (IP‐MS) assays. Both the IP‐MS and Simoa methods revealed that the use of P100 tubes significantly improves the stability of Aβ42 and Aβ40 across all approaches. However, the Aβ42/Aβ40 ratio levels were significantly stabilized only in the IP‐MS assay in Approach 3. No significant differences were observed in the levels of plasma p‐tau181, GFAP, and NfL for samples collected using either tube type in any of the approaches. Supplementation of blood collection tubes with protease inhibitors could reduce the protease‐induced degradation of plasma Aβ42 and Aβ40, and the Aβ42/40 ratio for the IP‐MS assay. These findings have crucial implications for preanalytical procedures, particularly in resource‐limited settings. [ABSTRACT FROM AUTHOR]

Published

2024

7. Harmonizing tau positron emission tomography in Alzheimer's disease: The CenTauR scale and the joint propagation model.

Author

Leuzy, Antoine, Raket, Lars Lau, Villemagne, Victor L., Klein, Gregory, Tonietto, Matteo, Olafson, Emily, Baker, Suzanne, Saad, Ziad S., Bullich, Santiago, Lopresti, Brian, Bohorquez, Sandra Sanabria, Boada, Mercè, Betthauser, Tobey J., Charil, Arnaud, Collins, Emily C., Collins, Jessica A., Cullen, Nicholas, Gunn, Roger N., Higuchi, Makoto, and Hostetler, Eric

Published

2024

8. Implementation and Assessment of Tau Thresholds in Non-Demented Individuals as Predictors of Cognitive Decline in Tau Imaging Studies.

Author

Gogola, Alexandra, Cohen, Ann D., Snitz, Beth, Minhas, Davneet, Tudorascu, Dana, Ikonomovic, Milos D., Shaaban, C. Elizabeth, Doré, Vincent, Matan, Cristy, Bourgeat, Pierrick, Mason, N. Scott, Leuzy, Antoine, Aizenstein, Howard, Mathis, Chester A., Lopez, Oscar L., Lopresti, Brian J., and Villemagne, Victor L.

Subjects

ALZHEIMER'S disease, TEMPORAL lobe, COGNITION disorders, DISEASE progression, TAU proteins

Abstract

Background: Tau accumulation in Alzheimer's disease is associated with short term clinical progression and faster rates of cognitive decline in individuals with high amyloid-β deposition. Defining an optimal threshold of tau accumulation predictive of cognitive decline remains a challenge. Objective: We tested the ability of regional tau PET sensitivity and specificity thresholds to predict longitudinal cognitive decline. We also tested the predictive performance of thresholds in the proposed new NIA-AA biological staging for Alzheimer's disease where multiple levels of tau positivity are used to stage participants. Methods: 18F-flortaucipir scans from 301 non-demented participants were processed and sampled. Four cognitive measures were assessed longitudinally. Regional standardized uptake value ratios were split into infra- and suprathreshold groups at baseline using previously derived thresholds. Survival analysis, log rank testing, and Generalized Estimation Equations assessed the relationship between the application of regional sensitivity/specificity thresholds and change in cognitive measures as well as tau threshold performance in predicting cognitive decline within the new NIA-AA biological staging. Results: The meta temporal region was best for predicting risk of short-term cognitive decline in suprathreshold, as compared to infrathreshold participants. When applying multiple levels of tau positivity, each subsequent level of tau identified cognitive decline at earlier timepoints. Conclusions: When using 18F-flortaucipir, meta temporal suprathreshold classification was associated with increased risk of cognitive decline, suggesting that abnormal tau deposition in the cortex predicts decline. Likewise, the application of multiple levels of tau clearly predicts the distinctive cognitive trajectories in the new NIA-AA biological staging framework. [ABSTRACT FROM AUTHOR]

Published

2024

9. Association of plasma biomarkers of Alzheimer's disease and related disorders with cognition and cognitive decline: The MYHAT population‐based study.

Author

Zhang, Yingjin, Ferreira, Pamela C. L., Jacobsen, Erin, Bellaver, Bruna, Pascoal, Tharick A., Snitz, Beth E., Chang, Chung‐Chou H., Villemagne, Victor L., Ganguli, Mary, and Karikari, Thomas K.

Published

2024

10. Alzheimer blood biomarkers: practical guidelines for study design, sample collection, processing, biobanking, measurement and result reporting.

Author

Zeng, Xuemei, Chen, Yijun, Sehrawat, Anuradha, Lee, Jihui, Lafferty, Tara K., Kofler, Julia, Berman, Sarah B., Sweet, Robert A., Tudorascu, Dana L., Klunk, William E., Ikonomovic, Milos D., Pfister, Anna, Zetterberg, Henrik, Snitz, Beth E., Cohen, Anne D., Villemagne, Victor L., Pascoal, Tharick A., Kamboh, M. llyas, Lopez, Oscar I., and Blennow, Kaj

Subjects

GLIAL fibrillary acidic protein, BIOMARKERS, ALZHEIMER'S disease, EXPERIMENTAL design, BLOOD collection

Abstract

Alzheimer's disease (AD), the most common form of dementia, remains challenging to understand and treat despite decades of research and clinical investigation. This might be partly due to a lack of widely available and cost-effective modalities for diagnosis and prognosis. Recently, the blood-based AD biomarker field has seen significant progress driven by technological advances, mainly improved analytical sensitivity and precision of the assays and measurement platforms. Several blood-based biomarkers have shown high potential for accurately detecting AD pathophysiology. As a result, there has been considerable interest in applying these biomarkers for diagnosis and prognosis, as surrogate metrics to investigate the impact of various covariates on AD pathophysiology and to accelerate AD therapeutic trials and monitor treatment effects. However, the lack of standardization of how blood samples and collected, processed, stored analyzed and reported can affect the reproducibility of these biomarker measurements, potentially hindering progress toward their widespread use in clinical and research settings. To help address these issues, we provide fundamental guidelines developed according to recent research findings on the impact of sample handling on blood biomarker measurements. These guidelines cover important considerations including study design, blood collection, blood processing, biobanking, biomarker measurement, and result reporting. Furthermore, the proposed guidelines include best practices for appropriate blood handling procedures for genetic and ribonucleic acid analyses. While we focus on the key blood-based AD biomarkers for the AT(N) criteria (e.g., amyloid-beta [Aβ]40, Aβ42, Aβ42/40 ratio, total-tau, phosphorylated-tau, neurofilament light chain, brain-derived tau and glial fibrillary acidic protein), we anticipate that these guidelines will generally be applicable to other types of blood biomarkers. We also anticipate that these guidelines will assist investigators in planning and executing biomarker research, enabling harmonization of sample handling to improve comparability across studies. [ABSTRACT FROM AUTHOR]

Published

2024

11. The AUstralian multidomain Approach to Reduce dementia Risk by prOtecting brain health With lifestyle intervention study (AU‐ARROW): A study protocol for a single‐blind, multi‐site, randomized controlled trial.

Author

Gardener, Samantha L., Fuller, Stephanie J., Naismith, Sharon L., Baker, Laura, Kivipelto, Miia, Villemagne, Victor L., Grieve, Stuart M., Yates, Paul, Rainey‐Smith, Stephanie R., Chen, Juliana, Thompson, Belinda, Armstrong, Nicola J., Fernando, Malika G., Blagojevic Castro, Carolina, Meghwar, Silochna, Raman, Rema, Gleason, Andrew, Ireland, Catriona, Clarnette, Roger, and Anstey, Kaarin J.

Subjects

DISEASE risk factors, POSITRON emission tomography, RESEARCH protocols, MAGNETIC resonance imaging, HEALTH education, BRAIN imaging, MEDITERRANEAN diet, COGNITIVE training

Abstract

INTRODUCTION: The Finnish Geriatric Intervention Study (FINGER) led to the global dementia risk reduction initiative: World‐Wide FINGERS (WW‐FINGERS). As part of WW‐FINGERS, the Australian AU‐ARROW study mirrors aspects of FINGER, as well as US‐POINTER. METHOD: AU‐ARROW is a randomized, single‐blind, multisite, 2‐year clinical trial (n = 600; aged 55–79). The multimodal lifestyle intervention group will engage in aerobic exercise, resistance training and stretching, dietary advice to encourage MIND diet adherence, BrainHQ cognitive training, and medical monitoring and health education. The Health Education and Coaching group will receive occasional health education sessions. The primary outcome measure is the change in a global composite cognitive score. Extra value will emanate from blood biomarker analysis, positron emission tomography (PET) imaging, brain magnetic resonance imaging (MRI), and retinal biomarker tests. DISCUSSION: The finalized AU‐ARROW protocol is expected to allow development of an evidence‐based innovative treatment plan to reduce cognitive decline and dementia risk, and effective transfer of research outcomes into Australian health policy. Highlights: Study protocol for a single‐blind, randomized controlled trial, the AU‐ARROW Study.The AU‐ARROW Study is a member of the World‐Wide FINGERS (WW‐FINGERS) initiative.AU‐ARROW's primary outcome measure is change in a global composite cognitive score.Extra significance from amyloid PET imaging, brain MRI, and retinal biomarker tests.Leading to development of an innovative treatment plan to reduce cognitive decline. [ABSTRACT FROM AUTHOR]

Published

2024

12. Suboptimal self‐reported sleep efficiency and duration are associated with faster accumulation of brain amyloid beta in cognitively unimpaired older adults.

Author

Pivac, Louise N., Brown, Belinda M., Sewell, Kelsey R., Doecke, James D., Villemagne, Victor L., Doré, Vincent, Weinborn, Michael, Sohrabi, Hamid R., Gardener, Samantha L., Bucks, Romola S., Laws, Simon M., Taddei, Kevin, Maruff, Paul, Masters, Colin L., Rowe, Christopher, Martins, Ralph N., and Rainey‐Smith, Stephanie R.

Subjects

SLEEP duration, OLDER people, AMYLOID, SLEEP quality, APOLIPOPROTEIN E, MIND-wandering, SLEEP

Abstract

INTRODUCTION: This study investigated whether self‐reported sleep quality is associated with brain amyloid beta (Aβ) accumulation. METHODS: Linear mixed effect model analyses were conducted for 189 cognitively unimpaired (CU) older adults (mean ± standard deviation 74.0 ± 6.2; 53.2% female), with baseline self‐reported sleep data, and positron emission tomography‐determined brain Aβ measured over a minimum of three time points (range 33.3–72.7 months). Analyses included random slopes and intercepts, interaction for apolipoprotein E (APOE) ε4 allele status, and time, adjusting for sex and baseline age. RESULTS: Sleep duration <6 hours, in APOE ε4 carriers, and sleep efficiency <65%, in the whole sample and APOE ε4 non‐carriers, is associated with faster accumulation of brain Aβ. DISCUSSION: These findings suggest a role for self‐reported suboptimal sleep efficiency and duration in the accumulation of Alzheimer's disease (AD) neuropathology in CU individuals. Additionally, poor sleep efficiency represents a potential route via which individuals at lower genetic risk may progress to preclinical AD. Highlights: In cognitively unimpaired older adults self‐report sleep is associated with brain amyloid beta (Aβ) accumulation.Across sleep characteristics, this relationship differs by apolipoprotein E (APOE) genotype.Sleep duration <6 hours is associated with faster brain Aβ accumulation in APOE ε4 carriers.Sleep efficiency < 65% is associated with faster brain Aβ accumulation in APOE ε4 non‐carriers.Personalized sleep interventions should be studied for potential to slow Aβ accumulation. [ABSTRACT FROM AUTHOR]

Published

2024

13. Brain 11β-Hydroxysteroid Dehydrogenase Type 1 Occupancy by Xanamem™ Assessed by PET in Alzheimer's Disease and Cognitively Normal Individuals.

Author

Villemagne, Victor L., Doré, Vincent, Chong, Lee, Kassiou, Michael, Mulligan, Rachel, Feizpour, Azadeh, Taylor, Jack, Roesner, Miriam, Miller, Tamara, and Rowe, Christopher C.

Subjects

ALZHEIMER'S disease, POSITRON emission tomography, MILD cognitive impairment, TEMPORAL lobe, BASAL ganglia

Abstract

Background: 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1) regulates intracellular cortisol and its inhibition by the small molecule inhibitor, Xanamem™, may provide a disease-modifying strategy for Alzheimer's disease (AD). Animal models suggest a range of 30–60% enzyme inhibition may suffice to provide neuroprotection. Objective: To determine the regional brain occupancy of 11β-HSD1 by Xanamem™ in cognitively normal participants (CN) and mild cognitive impairment (MCI)/mild AD patients to investigate potential dosing ranges for future efficacy studies. Methods: Seventeen MCI/AD and 23 CN were included. Regional brain time-activity curves (TAC), standardized uptake values (SUV40–60) and volume of distribution (VT) from Logan plot with image derived input function from 11C-TARACT positron emission tomography (PET) were used to assess the degree of 11β-HSD1 occupancy by increasing doses of Xanamem™ (5 mg, 10 mg, 20 mg or 30 mg daily for 7 days). Results: All measures showed high 11β-HSD1 occupancy with Xanamem to similar degree in CN and MCI/AD. The dose-response relationship was relatively flat above 5 mg. Respective median (interquartile range [Q1-Q3]) 11β-HSD1 occupancy in the MCI/AD and CN groups after treatment with 10 mg Xanamem were 80% [79–81%] and 75% [71–76%] in the neocortex, 69% [64–70%] and 61% [52–63%] in the medial temporal lobe, 80% [79–80%] and 73% [68–73%] in the basal ganglia, and 71% [67–75%] and 66% [62–68%] in the cerebellum. Conclusions: TAC, SUV40–60, and VT measures indicate Xanamem achieves high target occupancy levels with near saturation at 10 mg daily. These data support exploration of doses of≤10 mg daily in future clinical studies. [ABSTRACT FROM AUTHOR]

Published

2024

14. Physical activity and brain amyloid beta: A longitudinal analysis of cognitively unimpaired older adults.

Author

Slee, Michael G., Rainey‐Smith, Stephanie R., Villemagne, Victor L., Doecke, James D., Sohrabi, Hamid R., Taddei, Kevin, Ames, David, Dore, Vincent, Maruff, Paul, Laws, Simon M., Masters, Colin L., Rowe, Christopher C., Martins, Ralph N., Erickson, Kirk I., and Brown, Belinda M.

Published

2024

15. A novel ultrasensitive assay for plasma p‐tau217: Performance in individuals with subjective cognitive decline and early Alzheimer's disease.

Author

Gonzalez‐Ortiz, Fernando, Ferreira, Pamela C. L., González‐Escalante, Armand, Montoliu‐Gaya, Laia, Ortiz‐Romero, Paula, Kac, Przemyslaw R., Turton, Michael, Kvartsberg, Hlin, Ashton, Nicholas J., Zetterberg, Henrik, Harrison, Peter, Bellaver, Bruna, Povala, Guilherme, Villemagne, Victor L., Pascoal, Tharick A., Ganguli, Mary, Cohen, Anne D., Minguillon, Carolina, Contador, Jose, and Suárez‐Calvet, Marc

Published

2024

16. Sex‐dependent alterations in hippocampal connectivity are linked to cerebrovascular and amyloid pathologies in normal aging.

Author

Schweitzer, Noah, Li, Jinghang, Thurston, Rebecca C., Lopresti, Brian, Klunk, William E., Snitz, Beth, Tudorascu, Dana, Cohen, Ann, Kamboh, M. Ilyas, Halligan‐Eddy, Edythe, Iordanova, Bistra, Villemagne, Victor L., Aizenstein, Howard, and Wu, Minjie

Published

2024

17. Tau in dementia with Lewy bodies.

Author

Chin, Kai Sin, Churilov, Leonid, Doré, Vincent, Villemagne, Victor L, Rowe, Christopher C, Yassi, Nawaf, and Watson, Rosie

Subjects

ALZHEIMER'S disease diagnosis, BIOMARKERS, LEWY body dementia, CONFIDENCE intervals, TAU proteins, AMYLOID beta-protein precursor, DEMENTIA, POSITRON emission tomography, RESEARCH funding, DESCRIPTIVE statistics

Abstract

Objective: Neurofibrillary tangles are present in a proportion of people with dementia with Lewy bodies and may be associated with worse cognition. Recent advances in biomarkers for Alzheimer's disease include second-generation tau positron emission tomography as well as the detection of phosphorylated tau at threonine 181 (p-tau181) in plasma. This study aimed to investigate tau in people with dementia with Lewy bodies using a second-generation tau positron emission tomography tracer as well as plasma p-tau181. Methods: Twenty-seven participants (mean age 74.7 ± 5.5) with clinically diagnosed probable dementia with Lewy bodies underwent comprehensive clinical assessment and positron emission tomography imaging (18F-MK6240 and 18F-NAV4694). Plasma p-tau181 levels were measured using Simoa technology. Results: Five dementia with Lewy bodies participants (18.5%) had an abnormal tau positron emission tomography (increased tau uptake in the temporal meta-region-of-interest). Higher plasma p-tau181 concentrations correlated with higher tau deposition in the temporal region (ρ = 0.46, 95% confidence interval = [0.10, 0.72]) and classified abnormal tau positron emission tomography in dementia with Lewy bodies with an area under the curve of 0.95 (95% confidence interval = [0.86, 0.99]). Plasma p-tau181 also correlated positively with cortical amyloid-beta binding (ρ = 0.68, 95% confidence interval = [0.40, 0.84]) and classified abnormal amyloid-beta positron emission tomography in dementia with Lewy bodies with an area under the curve of 0.91 (95% confidence interval = [0.79, 0.99]). There was no association found between tau deposition and any of the clinical variables. Conclusions: Tau is a common co-pathology in dementia with Lewy bodies. Plasma p-tau181 correlated with abnormal tau and amyloid-beta positron emission tomography and may potentially be used as a marker to identify co-morbid Alzheimer's disease-related pathology in dementia with Lewy bodies. The clinical implications of tau in dementia with Lewy bodies need to be further evaluated in larger longitudinal studies. [ABSTRACT FROM AUTHOR]

Published

2024

18. Association Between β-Amyloid Accumulation and Incident Dementia in Individuals 80 Years or Older Without Dementia.

Author

Lopez, Oscar L., Villemagne, Victor L., Yue-Fang Chang, Cohen, Ann D., Klunk, William E., Mathis, Chester A., Pascoal, Tharick, Ikonomovic, Milos D., Rowe, Christopher, Dore, Vincent, Snitz, Beth E., Lopresti, Brian J., Kamboh, M. Ilyas, Aizenstein, Howard J., and Kuller, Lewis H.

Published

2024

19. A comparison of machine learning based‐composite cognitive test scores to track cognitive decline in early stages of Alzheimer's disease dementia: ADOPIC study.

Author

Shishegar, Rosita, Lee, Matthew, Cox, Timothy, Chai, Tze Young, Dore, Vincent, Bourgeat, Pierrick, Fripp, Jurgen, Burnham, Samantha C., Lamb, Fiona, Robertson, Joanne, Laws, Simon M, Porter, Tenielle, Savage, Greg, Hassenstab, Jason J., Morris, John C, Aschenbrenner, Andrew J., Weiner, Michael S. W., Masters, Colin L, Rowe, Christopher C, and Villemagne, Victor L

Published

2023

20. Amyloid β‐dependent tau phosphorylation is triggered by reactive astrocytes in preclinical Alzheimer's disease.

Author

Bellaver, Bruna, Povala, Guilherme, Ferreira, Pamela C.L., Ferrari‐Souza, João Pedro, Leffa, Douglas Teixeira, Lussier, Firoza Z, Benedet, Andrea Lessa, Ashton, Nicholas J., Tissot, Cécile, Therriault, Joseph, Servaes, Stijn, Stevenson, Jenna, Rahmouni, Nesrine, Lopez, Oscar L., Tudorascu, Dana, Villemagne, Victor L, Ikonomovic, Milos D, Gauthier, Serge, Zimmer, Eduardo R, and Zetterberg, Henrik

Published

2023

21. Amyloid β‐dependent tau phosphorylation is triggered by reactive astrocytes in preclinical Alzheimer's disease.

Author

Bellaver, Bruna, Povala, Guilherme, Ferreira, Pamela C.L., Ferrari‐Souza, João Pedro, Leffa, Douglas Teixeira, Lussier, Firoza Z, Benedet, Andrea Lessa, Ashton, Nicholas J., Tissot, Cécile, Therriault, Joseph, Servaes, Stijn, Stevenson, Jenna, Rahmouni, Nesrine, Lopez, Oscar L., Tudorascu, Dana, Villemagne, Victor L, Ikonomovic, Milos D, Gauthier, Serge, Zimmer, Eduardo R, and Zetterberg, Henrik

Published

2023

22. Using 18F-AV-133 VMAT2 PET Imaging to Monitor Progressive Nigrostriatal Degeneration in Parkinson Disease.

Author

Beauchamp, Leah C., Dore, Vincent, Villemagne, Victor L., Xu, SanSan, Finkelstein, David, Barnham, Kevin J., and Rowe, Christopher

Published

2023

23. Biostatistical Estimation of Tau Threshold Hallmarks (BETTH) Algorithm for Human Tau PET Imaging Studies.

Author

Gogola, Alexandra, Lopresti, Brian J., Tudorascu, Dana, Snitz, Beth, Minhas, Davneet, Doré, Vincent, Ikonomovic, Milos D., Shaaban, C. Elizabeth, Matan, Cristy, Bourgeat, Pierrick, Mason, N. Scott, Aizenstein, Howard, Mathis, Chester A., Klunk, William E., Rowe, Christopher C., Lopez, Oscar L., Cohen, Ann D., and Villemagne, Victor L.

Published

2023

24. Plasma biomarkers identify older adults at risk of Alzheimer's disease and related dementias in a real‐world population‐based cohort.

Author

Ferreira, Pamela C. L., Zhang, Yingjin, Snitz, Beth, Chang, Chung‐Chou H., Bellaver, Bruna, Jacobsen, Erin, Kamboh, M. Ilyas, Zetterberg, Henrik, Blennow, Kaj, Pascoal, Tharick A., Villemagne, Victor L., Ganguli, Mary, and Karikari, Thomas K.

Published

2023

25. Vesicular Glutamate Transporter Changes in the Cortical Default Mode Network During the Clinical and Pathological Progression of Alzheimer's Disease.

Author

Mi, Zhiping, Abrahamson, Eric E., Ryu, Angela Y., Malek-Ahmadi, Michael, Kofler, Julia K., Fish, Kenneth N., Sweet, Robert A., Villemagne, Victor L., Schneider, Julie A., Mufson, Elliott J., and Ikonomovic, Milos D.

Subjects

DEFAULT mode network, GLUTAMATE transporters, ALZHEIMER'S disease, DISEASE progression, MILD cognitive impairment

Abstract

Background: Altered glutamatergic neurotransmission may contribute to impaired default mode network (DMN) function in Alzheimer's disease (AD). Among the DMN hub regions, frontal cortex (FC) was suggested to undergo a glutamatergic plasticity response in prodromal AD, while the status of glutamatergic synapses in the precuneus (PreC) during clinical-neuropathological AD progression is not known. Objective: To quantify vesicular glutamate transporter VGluT1- and VGluT2-containing synaptic terminals in PreC and FC across clinical stages of AD. Methods: Unbiased sampling and quantitative confocal immunofluorescence of cortical VGluT1- and VGluT2-immunoreactive profiles and spinophilin-labeled dendritic spines were performed in cases with no cognitive impairment (NCI), mild cognitive impairment (MCI), mild-moderate AD (mAD), or moderate-severe AD (sAD). Results: In both regions, loss of VGluT1-positive profile density was seen in sAD compared to NCI, MCI, and mAD. VGluT1-positive profile intensity in PreC did not differ across groups, while in FC it was greater in MCI, mAD, and sAD compared to NCI. VGluT2 measures were stable in PreC while FC had greater VGluT2-positive profile density in MCI compared to sAD, but not NCI or mAD. Spinophilin measures in PreC were lower in mAD and sAD compared to NCI, while in FC they were stable across groups. Lower VGluT1 and spinophilin measures in PreC, but not FC, correlated with greater neuropathology. Conclusion: Frank loss of VGluT1 in advanced AD relative to NCI occurs in both DMN regions. In FC, an upregulation of VGluT1 protein content in remaining glutamatergic terminals may contribute to this region's plasticity response in AD. [ABSTRACT FROM AUTHOR]

Published

2023

26. A universal neocortical mask for Centiloid quantification.

Author

Bourgeat, Pierrick, Doré, Vincent, Rowe, Christopher C., Benzinger, Tammie, Tosun, Duygu, Goyal, Manu S., LaMontagne, Pamela, Jin, Liang, Weiner, Michael W., Masters, Colin L., Fripp, Jurgen, and Villemagne, Victor L.

Subjects

POSITRON emission tomography, ALZHEIMER'S disease, MILD cognitive impairment

Abstract

INTRODUCTION: The Centiloid (CL) project was developed to harmonize the quantification of amyloid beta (Aβ) positron emission tomography (PET) scans to a unified scale. The CL neocortical mask was defined using 11C Pittsburgh compound B (PiB), overlooking potential differences in regional distribution among Aβ tracers. We created a universal mask using an independent dataset of five Aβ tracers, and investigated its impact on inter‐tracer agreement, tracer variability, and group separation. METHODS: Using data from the Alzheimer's Dementia Onset and Progression in International Cohorts (ADOPIC) study (Australian Imaging Biomarkers and Lifestyle + Alzheimer's Disease Neuroimaging Initiative + Open Access Series of Imaging Studies), age‐matched pairs of mild Alzheimer's disease (AD) and healthy controls (HC) were selected: 18F‐florbetapir (N = 147 pairs), 18F‐florbetaben (N = 22), 18F‐flutemetamol (N = 10), 18F‐NAV (N = 42), 11C‐PiB (N = 63). The images were spatially and standardized uptake value ratio normalized. For each tracer, the mean AD–HC difference image was thresholded to maximize the overlap with the standard neocortical mask. The universal mask was defined as the intersection of all five masks. It was evaluated on the Global Alzheimer's Association Interactive Network (GAAIN) head‐to‐head datasets in terms of inter‐tracer agreement and variance in the young controls (YC) and on the ADOPIC dataset comparing separation between HC/AD and HC/mild cognitive impairment (MCI). RESULTS: In the GAAIN dataset, the universal mask led to a small reduction in the variance of the YC, and a small increase in the inter‐tracer agreement. In the ADOPIC dataset, it led to a better separation between HC/AD and HC/MCI at baseline. DISCUSSION: The universal CL mask led to an increase in inter‐tracer agreement and group separation. Those increases were, however, very small, and do not provide sufficient benefits to support departing from the existing standard CL mask, which is suitable for the quantification of all Aβ tracers. HIGHLIGHTS: This study built an amyloid universal mask using a matched cohort for the five most commonly used amyloid positron emission tomography tracers.There was a high overlap between each tracer‐specific mask.Differences in quantification and group separation between the standard and universal mask were small.The existing standard Centiloid mask is suitable for the quantification of all amyloid beta tracers. [ABSTRACT FROM AUTHOR]

Published

2023

27. CenTauR: Toward a universal scale and masks for standardizing tau imaging studies.

Author

Villemagne, Victor L., Leuzy, Antoine, Bohorquez, Sandra Sanabria, Bullich, Santiago, Shimada, Hitoshi, Rowe, Christopher C., Bourgeat, Pierrick, Lopresti, Brian, Huang, Kun, Krishnadas, Natasha, Fripp, Jurgen, Takado, Yuhei, Gogola, Alexandra, Minhas, Davneet, Weimer, Robby, Higuchi, Makoto, Stephens, Andrew, Hansson, Oskar, and Doré, Vincent

Subjects

DIAGNOSTIC imaging, ALZHEIMER'S disease

Abstract

INTRODUCTION: Recently, an increasing number of tau tracers have become available. There is a need to standardize quantitative tau measures across tracers, supporting a universal scale. We developed several cortical tau masks and applied them to generate a tau imaging universal scale. METHOD: One thousand forty‐five participants underwent tau scans with either 18F‐flortaucipir, 18F‐MK6240, 18F‐PI2620, 18F‐PM‐PBB3, 18F‐GTP1, or 18F‐RO948. The universal mask was generated from cognitively unimpaired amyloid beta (Aβ)− subjects and Alzheimer's disease (AD) patients with Aβ+. Four additional regional cortical masks were defined within the constraints of the universal mask. A universal scale, the CenTauRz, was constructed. RESULTS: None of the regions known to display off‐target signal were included in the masks. The CenTauRz allows robust discrimination between low and high levels of tau deposits. DISCUSSION: We constructed several tau‐specific cortical masks for the AD continuum and a universal standard scale designed to capture the location and degree of abnormality that can be applied across tracers and across centers. The masks are freely available at https://www.gaain.org/centaur‐project. [ABSTRACT FROM AUTHOR]

Published

2023

28. Exploring how genetic variation within Aquaporin‐4, influences the relationship between sleep and amyloid beta.

Author

Porter, Tenielle, Armstrong, Ayeisha Milligan, Dore, Vincent, O'Brien, Eleanor K., Bourgeat, Pierrick, Maruff, Paul, Rowe, Christopher C., Smith, Stephanie Rainey, Villemagne, Victor L, and Laws, Simon M.

Published

2024

29. Polygenic scores for Alzheimer's disease risk and resilience predict age at onset of amyloid‐β.

Author

O'Brien, Eleanor K., Porter, Tenielle, Fernandez, Shane, Cox, Timothy, Dore, Vincent, Bourgeat, Pierrick, Goudey, Benjamin, Doecke, James D., Masters, Colin L., Rowe, Christopher C., Villemagne, Victor L, Cruchaga, Carlos, Saykin, Andrew J., and Laws, Simon M

Published

2024

30. The flutemetamol analogue cyano-flutemetamol detects myocardial AL and ATTR amyloid deposits: a post-mortem histofluorescence analysis.

Author

Abrahamson, Eric E., Padera, Robert F., Davies, Julie, Farrar, Gill, Villemagne, Victor L., Dorbala, Sharmila, and Ikonomovic, Milos D.

Subjects

AMYLOID plaque, IMMUNOGLOBULIN light chains, POSITRON emission tomography, CARDIAC amyloidosis, CARDIAC magnetic resonance imaging

Abstract

[18F]flutemetamol is a PET radioligand used to image brain amyloid, but its detection of myocardial amyloid is not well-characterized. This histological study characterized binding of fluorescently labeled flutemetamol (cyano-flutemetamol) to amyloid deposits in myocardium. Myocardial tissue was obtained post-mortem from 29 subjects with cardiac amyloidosis including transthyretin wild-type (ATTRwt), hereditary/variant transthyretin (ATTRv) and immunoglobulin light-chain (AL) types, and from 10 cardiac amyloid-free controls. Most subjects had antemortem electrocardiography, echocardiography, SPECT and cardiac MRI. Cyano-flutemetamol labeling patterns and integrated density values were evaluated relative to fluorescent derivatives of Congo red (X-34) and Pittsburgh compound-B (cyano-PiB). Cyano-flutemetamol labeling was not detectable in control subjects. In subjects with cardiac amyloidosis, cyano-flutemetamol labeling matched X-34- and cyano-PiB-labeled, and transthyretin- or lambda light chain-immunoreactive, amyloid deposits and was prevented by formic acid pre-treatment of myocardial sections. Cyano-flutemetamol mean fluorescence intensity, when adjusted for X-34 signal, was higher in the ATTRwt than the AL group. Cyano-flutemetamol integrated density correlated strongly with echocardiography measures of ventricular septal thickness and posterior wall thickness, and with heart mass. The high selectivity of cyano-flutemetamol binding to myocardial amyloid supports the diagnostic utility of [18F]flutemetamol PET imaging in patients with ATTR and AL types of cardiac amyloidosis. [ABSTRACT FROM AUTHOR]

Published

2023

31. Tau, β-Amyloid, and Glucose Metabolism Following Service-Related Traumatic Brain Injury in Vietnam War Veterans: The Australian Imaging Biomarkers and Lifestyle Study of Aging-Veterans Study (AIBL-VETS).

Author

Cummins, Tia L., Doré, Vincent, Feizpour, Azadeh, Krishnadas, Natasha, Bourgeat, Pierrick, Elias, Alby, Lamb, Fiona, Williams, Robert, Hopwood, Malcolm, Landau, Susan, Villemagne, Victor L., Weiner, Michael, and Rowe, Christopher C.

Published

2023

32. Plasma Aβ42/40 ratio, p‐tau181, GFAP, and NfL across the Alzheimer's disease continuum: A cross‐sectional and longitudinal study in the AIBL cohort.

Author

Chatterjee, Pratishtha, Pedrini, Steve, Doecke, James D., Thota, Rohith, Villemagne, Victor L., Doré, Vincent, Singh, Abhay K., Wang, Penghao, Rainey‐Smith, Stephanie, Fowler, Christopher, Taddei, Kevin, Sohrabi, Hamid R., Molloy, Mark P., Ames, David, Maruff, Paul, Rowe, Christopher C., Masters, Colin L., and Martins, Ralph N.

Published

2023

33. Association between amyloid-beta deposition and cortical thickness in dementia with Lewy bodies.

Author

Chin, Kai Sin, Gajamange, Sanuji, Desmond, Patricia M, Villemagne, Victor L, Rowe, Christopher C, Churilov, Leonid, Yassi, Nawaf, and Watson, Rosie

Subjects

LEWY body dementia, ALZHEIMER'S disease, HIPPOCAMPUS (Brain), SCIENTIFIC observation, CONFIDENCE intervals, MAGNETIC resonance imaging, AMYLOID beta-protein precursor, BRAIN cortical thickness, PSYCHOLOGICAL tests, T-test (Statistics), POSITRON emission tomography, DESCRIPTIVE statistics, QUESTIONNAIRES, RESEARCH funding, SENSITIVITY & specificity (Statistics), DATA analysis software, ODDS ratio, RECEIVER operating characteristic curves

Abstract

Objective: Amyloid-beta often co-exists in dementia with Lewy bodies, but its clinical relevance in dementia with Lewy bodies remains unclear. This study aimed to investigate the clinical and imaging correlates of amyloid-beta deposition in dementia with Lewy bodies, particularly its relationship with cortical thickness in Alzheimer's disease–prone regions and hippocampal volume. Methods: Twenty-four participants with probable dementia with Lewy bodies underwent high-resolution magnetic resonance imaging and amyloid-beta positron emission tomography imaging using the radiotracer 18F-NAV4694. Amyloid-beta deposition was quantified and reported using the Centiloid method. Results: Amyloid-beta positivity, defined as Centiloid > 50, was present in 45.8% of dementia with Lewy bodies participants. There were no statistically significant differences in clinical characteristics between Aβ+ and Aβ− dementia with Lewy bodies. Compared with the Aβ− group, Aβ+ dementia with Lewy bodies exhibited greater global cortical thinning as well as in the Alzheimer's disease–prone region of interest, adjusted for age, sex and years of education. A mean cortical thickness of 5.12 mm across a combined meta-region of interest has a sensitivity of 88.9% and specificity of 90.0% in discriminating Aβ+ from Aβ− dementia with Lewy bodies. Hippocampal volume was not different between groups. Conclusion: Early structural changes in cortical thickness, but not hippocampal volume, were observed in dementia with Lewy bodies with significant amyloid-beta burden. This may represent an early Alzheimer's disease–related neurodegenerative process. [ABSTRACT FROM AUTHOR]

Published

2023

34. Associations of mid‐life cardiovascular function with late‐life Alzheimer's disease pathology burden in the Heart SCORE study.

Author

Royse, Sarah K., Saeed, Anum, Reese, Alexandria C., Lopresti, Brian J., Snitz, Beth E., Villemagne, Victor L, Nadkarni, Neelesh K., Reis, Steven E., Lopez, Oscar L., and Cohen, Ann D.

Published

2023

35. Increased Genetic Risk for ADHD Potentiates Cognitive Impairment and Brain Hypometabolism in Alzheimer's Disease Patients.

Author

Leffa, Douglas Teixeira, Povala, Guilherme, Bellaver, Bruna, Lussier, Firoza Z, Ferrari‐Souza, João Pedro, Ferreira, Pamela C.L., Zalzale, Hussein, Aguzzoli, Cristiano Schaffer, Rohden, Francieli, Soares, Carolina, Abbas, Sarah, Tissot, Cécile, Therriault, Joseph, Lopez, Oscar L., Villemagne, Victor L, Klunk, William E, Cohen, Annie, Zimmer, Eduardo R., Karikari, Thomas K, and Rosa‐Neto, Pedro

Published

2023

36. The effect of basal forebrain atrophy on the rate of cognitive decline in older adults without dementia.

Author

Xia, Ying, Maruff, Paul, Dore, Vincent, Bourgeat, Pierrick, Villemagne, Victor L, Rowe, Christopher C, Coulson, Elizabeth J, and Fripp, Jurgen

Published

2023

37. Astrocyte reactivity potentiates longitudinal tau tangle accumulation in cognitively unimpaired individuals.

Author

Bellaver, Bruna, Povala, Guilherme, Ferreira, Pamela C.L., Ferrari‐Souza, João Pedro, Leffa, Douglas Teixeira, Lussier, Firoza Z, Zalzale, Hussein, Soares, Carolina, Aguzzoli, Cristiano Schaffer, Rohden, Francieli, Abbas, Sarah, Ashton, Nicholas J., Tissot, Cécile, Therriault, Joseph, Servaes, Stijn, Stevenson, Jenna, Rahmouni, Nesrine, Lopez, Oscar L., Tudorascu, Dana, and Villemagne, Victor L

Published

2023

38. Risk architecture for altered hippocampal connectivity in normal aging differ between men and women.

Author

Schweitzer, Noah, Li, Jinghang, Lopresti, Brian J, Klunk, William E, Snitz, Beth E., Tudorascu, Dana, Cohen, Ann D., Kamboh, M. Ilyas, Halligan, Edye, Thurston, Rebecca C, Villemagne, Victor L, Iordanova, Bistra, Aizenstein, Howard J, and Wu, Minjie

Published

2023

39. A CenTauR scale based on 18F‐MK6240.

Author

Dore, Vincent, Bourgeat, Pierrick, Leuzy, Antoine, Huang, Kun, Krishnadas, Natasha, Feizpour, Azadeh, Fripp, Jurgen, Villemagne, Victor L, and Rowe, Christopher C

Published

2023

40. Assessing a universal neocortical mask for Centiloid quantification.

Author

Bourgeat, Pierrick, Dore, Vincent, Rowe, Christopher C, Benzinger, Tammie L.S., Tosun, Duygu, Goyal, Manu S., LaMontagne, Pamela J., Jin, Liang, Weiner, Michael S. W., Morris, John C, Masters, Colin L, Fripp, Jurgen, and Villemagne, Victor L

Published

2023

41. Plasma p‐tau181 and nfl as surrogates biomarkers in clinical trials targeting preclinical stage of Alzheimer's disease.

Author

Ferreira, Pamela C.L., Ferrari‐Souza, João Pedro, Tissot, Cécile, Bellaver, Bruna, Leffa, Douglas Teixeira, Povala, Guilherme, Lussier, Firoza Z, Therriault, Joseph, Benedet, Andrea Lessa, Ashton, Nicholas J., Cohen, Ann D., Lopez, Oscar L., Tudorascu, Dana, Klunk, William E, Soucy, Jean‐Paul, Gauthier, Serge, Villemagne, Victor L, Zetterberg, Henrik, Blennow, Kaj, and Rosa‐Neto, Pedro

Published

2023

42. Plasma p‐tau181 and nfl as surrogates biomarkers in clinical trials targeting preclinical stage of Alzheimer's disease.

Author

Ferreira, Pamela C.L., Ferrari‐Souza, João Pedro, Tissot, Cécile, Bellaver, Bruna, Leffa, Douglas Teixeira, Povala, Guilherme, Lussier, Firoza Z, Therriault, Joseph, Benedet, Andrea Lessa, Ashton, Nicholas J., Cohen, Ann D., Lopez, Oscar L., Tudorascu, Dana, Klunk, William E, Soucy, Jean‐Paul, Gauthier, Serge, Villemagne, Victor L, Zetterberg, Henrik, Blennow, Kaj, and Rosa‐Neto, Pedro

Published

2023

43. A CenTauR scale based on 18F‐MK6240.

Author

Dore, Vincent, Bourgeat, Pierrick, Leuzy, Antoine, Huang, Kun, Krishnadas, Natasha, Feizpour, Azadeh, Fripp, Jurgen, Villemagne, Victor L, and Rowe, Christopher C

Published

2023

44. Assessing a universal neocortical mask for Centiloid quantification.

Author

Bourgeat, Pierrick, Dore, Vincent, Rowe, Christopher C, Benzinger, Tammie L.S., Tosun, Duygu, Goyal, Manu S., LaMontagne, Pamela J., Jin, Liang, Weiner, Michael S. W., Morris, John C, Masters, Colin L, Fripp, Jurgen, and Villemagne, Victor L

Published

2023

45. Plasma Glial Fibrillary Acidic Protein Is Associated with 18F-SMBT-1 PET: Two Putative Astrocyte Reactivity Biomarkers for Alzheimer's Disease.

Author

Chatterjee, Pratishtha, Doré, Vincent, Pedrini, Steve, Krishnadas, Natasha, Thota, Rohith, Bourgeat, Pierrick, Ikonomovic, Milos D., Rainey-Smith, Stephanie R., Burnham, Samantha C., Fowler, Christopher, Taddei, Kevin, Mulligan, Rachel, Ames, David, Masters, Colin L., Fripp, Jürgen, Rowe, Christopher C., Martins, Ralph N., and Villemagne, Victor L.

Subjects

GLIAL fibrillary acidic protein, ALZHEIMER'S disease, PARIETAL lobe, CINGULATE cortex, BIOMARKERS

Abstract

Background: Astrocyte reactivity is an early event along the Alzheimer's disease (AD) continuum. Plasma glial fibrillary acidic protein (GFAP), posited to reflect astrocyte reactivity, is elevated across the AD continuum from preclinical to dementia stages. Monoamine oxidase-B (MAO-B) is also elevated in reactive astrocytes observed using 18F-SMBT-1 PET in AD. Objective: The objective of this study was to evaluate the association between the abovementioned astrocyte reactivity biomarkers. Methods: Plasma GFAP and Aβ were measured using the Simoa® platform in participants who underwent brain 18F-SMBT-1 and Aβ–PET imaging, comprising 54 healthy control (13 Aβ–PET+ and 41 Aβ–PET–), 11 mild cognitively impaired (3 Aβ–PET+ and 8 Aβ–PET–) and 6 probable AD (5 Aβ–PET+ and 1 Aβ–PET–) individuals. Linear regressions were used to assess associations of interest. Results: Plasma GFAP was associated with 18F-SMBT-1 signal in brain regions prone to early Aβ deposition in AD, such as the supramarginal gyrus (SG), posterior cingulate (PC), lateral temporal (LT) and lateral occipital cortex (LO). After adjusting for age, sex, APOE ɛ4 genotype, and soluble Aβ (plasma Aβ42/40 ratio), plasma GFAP was associated with 18F-SMBT-1 signal in the SG, PC, LT, LO, and superior parietal cortex (SP). On adjusting for age, sex, APOE ɛ4 genotype and insoluble Aβ (Aβ–PET), plasma GFAP was associated with 18F-SMBT-1 signal in the SG. Conclusion: There is an association between plasma GFAP and regional 18F-SMBT-1 PET, and this association appears to be dependent on brain Aβ load. [ABSTRACT FROM AUTHOR]

Published

2023

46. EDITOR SPOTLIGHT: Interview with Brain Imaging Special Issue guest editors Victor Villemagne and Yulong Li.

Author

Kwan, Kim H., Villemagne, Victor L., and Li, Yulong

Subjects

BRAIN imaging, CAREER development, ALZHEIMER'S disease, NEUROSCIENCES, SEROTONIN

Published

2023

47. Preclinical and clinical imaging techniques as pathophysiological biomarkers — A preface to the special issue "Brain Imaging".

Author

Villemagne, Victor L. and Li, Yulong

Subjects

BRAIN imaging, DIAGNOSTIC imaging, BIOMARKERS, POSITRON emission tomography, MOLECULAR dynamics

Abstract

Molecular imaging techniques have become important tools to characterize and measure biological processes at the cellular and molecular levels. Nowadays, molecular imaging techniques are widely used in preclinical and clinical studies to assess the molecular dynamics under physiological conditions and during pathological processes. This special issue on Brain Imaging (https://onlinelibrary.wiley.com/doi/toc/10.1111/[ISSN]1471‐4159.brain‐imaging) will highlight some of the recent advances in developing new tools and applying molecular imaging techniques to understand biomarker dynamics in health and diseases. [ABSTRACT FROM AUTHOR]

Published

2023

48. Comparison of plasma amyloid, tau, and astrocyte biomarkers to identify AD pathophysiology.

Author

Ferreira, Pamela C.L., Tissot, Cécile, Ferrari‐Souza, João Pedro, Bellaver, Bruna, Brum, Wagner S., Leffa, Douglas Teixeira, Therriault, Joseph, Benedet, Andréa Lessa, Servaes, Stijn, Lussier, Firoza Z, Chamoun, Mira, Stevenson, Jenna, Rahmouni, Nesrine, Tudorascu, Dana L, Klunk, William E, Villemagne, Victor L, Cohen, Ann D, Zimmer, Eduardo R., Ashton, Nicholas J., and Zetterberg, Henrik

Published

2022

49. Cross‐sectional and longitudinal comparison of 18F‐MK6240 and 18F‐Flortaucipir in populations matched for centiloid, age and MMSE.

Author

Bourgeat, Pierrick, Krishnadas, Natasha, Dore, Vincent, Mulligan, Rachel S, Tyrrell, Regan, Bozinovski, Svetlana, Huang, Kun, Lamb, Fiona, Fripp, Jurgen, Villemagne, Victor L, and Rowe, Christopher

Published

2022

50. Comparison of plasma amyloid, tau, and astrocyte biomarkers to identify AD pathophysiology.

Author

Ferreira, Pamela C.L., Tissot, Cécile, Ferrari‐Souza, João Pedro, Bellaver, Bruna, Brum, Wagner S., Leffa, Douglas Teixeira, Therriault, Joseph, Benedet, Andréa Lessa, Servaes, Stijn, Lussier, Firoza Z, Chamoun, Mira, Stevenson, Jenna, Rahmouni, Nesrine, Tudorascu, Dana L, Klunk, William E, Villemagne, Victor L, Cohen, Ann D, Zimmer, Eduardo R., Ashton, Nicholas J., and Zetterberg, Henrik

Published

2022