Your search keyword '"Leuzy A"' showing total 44 results

1. [18F]RO948 tau positron emission tomography in genetic and sporadic frontotemporal dementia syndromes.

Author

Santillo, Alexander F., Leuzy, Antoine, Honer, Michael, Landqvist Waldö, Maria, Tideman, Pontus, Harper, Luke, Ohlsson, Tomas, Moes, Svenja, Giannini, Lucia, Jögi, Jonas, Groot, Colin, Ossenkoppele, Rik, Strandberg, Olof, van Swieten, John, Smith, Ruben, and Hansson, Oskar

Subjects

*DIAGNOSIS of dementia, *POSITRON emission tomography, *NEUROLOGICAL disorders, *AUTORADIOGRAPHY, *PROTEINS

Abstract

Purpose: To examine [18F]RO948 retention in FTD, sampling the underlying protein pathology heterogeneity. Methods: A total of 61 individuals with FTD (n = 35), matched cases of AD (n = 13) and Aβ-negative cognitively unimpaired individuals (n = 13) underwent [18F]RO948PET and MRI. FTD included 21 behavioral variant FTD (bvFTD) cases, 11 symptomatic C9orf72 mutation carriers, one patient with non-genetic bvFTD-ALS, one individual with bvFTD due to a GRN mutation, and one due to a MAPT mutation (R406W). Tracer retention was examined using a region-of-interest and voxel-wise approaches. Two individuals (bvFTD due to C9orf72) underwent postmortem neuropathological examination. Tracer binding was additionally assessed in vitro using [3H]RO948 autoradiography in six separate cases. Results: [18F]RO948 retention across ROIs was clearly lower than in AD and comparable to that in Aβ-negative cognitively unimpaired individuals. Only minor loci of tracer retention were seen in bvFTD; these did not overlap with the observed cortical atrophy in the cases, the expected pattern of atrophy, nor the expected or verified protein pathology distribution. Autoradiography analyses showed no specific [3H]RO948 binding. The R406W MAPT mutation carriers were clear exceptions with AD-like retention levels and specific in-vitro binding. Conclusion: [18F]RO948 uptake is not significantly increased in the majority of FTD patients, with a clear exception being specific MAPT mutations. [ABSTRACT FROM AUTHOR]

Published

2023

2. The validation status of blood biomarkers of amyloid and phospho-tau assessed with the 5-phase development framework for AD biomarkers.

Author

Ashton, N. J., Leuzy, A., Karikari, T. K., Mattsson-Carlgren, N., Dodich, A., Boccardi, M., Corre, J., Drzezga, A., Nordberg, A., Ossenkoppele, R., Zetterberg, H., Blennow, K., Frisoni, G. B., Garibotto, V., and Hansson, O.

Subjects

*CEREBROSPINAL fluid examination, *POSITRON emission tomography, *BIOMARKERS, *TAU proteins, *AMYLOID, *CEREBROSPINAL fluid, *ALZHEIMER'S disease

Abstract

Purpose: The development of blood biomarkers that reflect Alzheimer's disease (AD) pathophysiology (phosphorylated tau and amyloid-β) has offered potential as scalable tests for dementia differential diagnosis and early detection. In 2019, the Geneva AD Biomarker Roadmap Initiative included blood biomarkers in the systematic validation of AD biomarkers. Methods: A panel of experts convened in November 2019 at a two-day workshop in Geneva. The level of maturity (fully achieved, partly achieved, preliminary evidence, not achieved, unsuccessful) of blood biomarkers was assessed based on the Biomarker Roadmap methodology and discussed fully during the workshop which also evaluated cerebrospinal fluid (CSF) and positron emission tomography (PET) biomarkers. Results: Plasma p-tau has shown analytical validity (phase 2 primary aim 1) and first evidence of clinical validity (phase 3 primary aim 1), whereas the maturity level for Aβ remains to be partially achieved. Full and partial achievement has been assigned to p-tau and Aβ, respectively, in their associations to ante-mortem measures (phase 2 secondary aim 2). However, only preliminary evidence exists for the influence of covariates, assay comparison and cut-off criteria. Conclusions: Despite the relative infancy of blood biomarkers, in comparison to CSF biomarkers, much has already been achieved for phases 1 through 3 – with p-tau having greater success in detecting AD and predicting disease progression. However, sufficient data about the effect of covariates on the biomarker measurement is lacking. No phase 4 (real-world performance) or phase 5 (assessment of impact/cost) aim has been tested, thus not achieved. [ABSTRACT FROM AUTHOR]

Published

2021

3. A multicenter comparison of [18F]flortaucipir, [18F]RO948, and [18F]MK6240 tau PET tracers to detect a common target ROI for differential diagnosis.

Author

Leuzy, Antoine, Pascoal, Tharick A., Strandberg, Olof, Insel, Philip, Smith, Ruben, Mattsson-Carlgren, Niklas, Benedet, Andréa L., Cho, Hannah, Lyoo, Chul H., La Joie, Renaud, Rabinovici, Gil D., Ossenkoppele, Rik, Rosa-Neto, Pedro, and Hansson, Oskar

Subjects

*RECEIVER operating characteristic curves, *DIFFERENTIAL diagnosis, *POSITRON emission tomography, *HIERARCHICAL clustering (Cluster analysis)

Abstract

Purpose: This study aims to determine whether comparable target regions of interest (ROIs) and cut-offs can be used across [18F]flortaucipir, [18F]RO948, and [18F]MK6240 tau positron emission tomography (PET) tracers for differential diagnosis of Alzheimer's disease (AD) dementia vs either cognitively unimpaired (CU) individuals or non-AD neurodegenerative diseases. Methods: A total of 1755 participants underwent tau PET using either [18F]flortaucipir (n = 975), [18F]RO948 (n = 493), or [18F]MK6240 (n = 287). SUVR values were calculated across four theory-driven ROIs and several tracer-specific data-driven (hierarchical clustering) regions of interest (ROIs). Diagnostic performance and cut-offs for ROIs were determined using receiver operating characteristic analyses and the Youden index, respectively. Results: Comparable diagnostic performance (area under the receiver operating characteristic curve [AUC]) was observed between theory- and data-driven ROIs. The theory-defined temporal meta-ROI generally performed very well for all three tracers (AUCs: 0.926–0.996). An SUVR value of approximately 1.35 was a common threshold when using this ROI. Conclusion: The temporal meta-ROI can be used for differential diagnosis of dementia patients with [18F]flortaucipir, [18F]RO948, and [18F]MK6240 tau PET with high accuracy, and that using very similar cut-offs of around 1.35 SUVR. This ROI/SUVR cut-off can also be applied across tracers to define tau positivity. [ABSTRACT FROM AUTHOR]

Published

2021

4. 2020 update on the clinical validity of cerebrospinal fluid amyloid, tau, and phospho-tau as biomarkers for Alzheimer's disease in the context of a structured 5-phase development framework.

Author

Leuzy, A., Ashton, N. J., Mattsson-Carlgren, N., Dodich, A., Boccardi, M., Corre, J., Drzezga, A., Nordberg, A., Ossenkoppele, R., Zetterberg, H., Blennow, K., Frisoni, G. B., Garibotto, V., and Hansson, O.

Subjects

*ALZHEIMER'S disease, *CEREBROSPINAL fluid, *TAU proteins, *BIOMARKERS, *AMYLOID

Abstract

Purpose: In the last decade, the research community has focused on defining reliable biomarkers for the early detection of Alzheimer's disease (AD) pathology. In 2017, the Geneva AD Biomarker Roadmap Initiative adapted a framework for the systematic validation of oncological biomarkers to cerebrospinal fluid (CSF) AD biomarkers—encompassing the 42 amino-acid isoform of amyloid-β (Aβ42), phosphorylated-tau (P-tau), and Total-tau (T-tau)—with the aim to accelerate their development and clinical implementation. The aim of this work is to update the current validation status of CSF AD biomarkers based on the Biomarker Roadmap methodology. Methods: A panel of experts in AD biomarkers convened in November 2019 at a 2-day workshop in Geneva. The level of maturity (fully achieved, partly achieved, preliminary evidence, not achieved, unsuccessful) of CSF AD biomarkers was assessed based on the Biomarker Roadmap methodology before the meeting and presented and discussed during the workshop. Results: By comparison to the previous 2017 Geneva Roadmap meeting, the primary advances in CSF AD biomarkers have been in the area of a unified protocol for CSF sampling, handling and storage, the introduction of certified reference methods and materials for Aβ42, and the introduction of fully automated assays. Additional advances have occurred in the form of defining thresholds for biomarker positivity and assessing the impact of covariates on their discriminatory ability. Conclusions: Though much has been achieved for phases one through three, much work remains in phases four (real world performance) and five (assessment of impact/cost). To a large degree, this will depend on the availability of disease-modifying treatments for AD, given these will make accurate and generally available diagnostic tools key to initiate therapy. [ABSTRACT FROM AUTHOR]

Published

2021

5. The impact of demographic, clinical, genetic, and imaging variables on tau PET status.

Author

Ossenkoppele, Rik, Leuzy, Antoine, Cho, Hanna, Sudre, Carole H., Strandberg, Olof, Smith, Ruben, Palmqvist, Sebastian, Mattsson-Carlgren, Niklas, Olsson, Tomas, Jögi, Jonas, Stormrud, Erik, Ryu, Young Hoon, Choi, Jae Yong, Boxer, Adam L., Gorno-Tempini, Maria L., Miller, Bruce L., Soleimani-Meigooni, David, Iaccarino, Leonardo, La Joie, Renaud, and Borroni, Edilio

Subjects

*TAU proteins, *ENTORHINAL cortex, *ALZHEIMER'S disease, *MILD cognitive impairment, *DEMENTIA, *WHITE matter (Nerve tissue)

Abstract

Purpose: A substantial proportion of amyloid-β (Aβ)+ patients with clinically diagnosed Alzheimer's disease (AD) dementia and mild cognitive impairment (MCI) are tau PET–negative, while some clinically diagnosed non-AD neurodegenerative disorder (non-AD) patients or cognitively unimpaired (CU) subjects are tau PET–positive. We investigated which demographic, clinical, genetic, and imaging variables contributed to tau PET status. Methods: We included 2338 participants (430 Aβ+ AD dementia, 381 Aβ+ MCI, 370 non-AD, and 1157 CU) who underwent [18F]flortaucipir (n = 1944) or [18F]RO948 (n = 719) PET. Tau PET positivity was determined in the entorhinal cortex, temporal meta-ROI, and Braak V-VI regions using previously established cutoffs. We performed bivariate binary logistic regression models with tau PET status (positive/negative) as dependent variable and age, sex, APOEε4, Aβ status (only in CU and non-AD analyses), MMSE, global white matter hyperintensities (WMH), and AD-signature cortical thickness as predictors. Additionally, we performed multivariable binary logistic regression models to account for all other predictors in the same model. Results: Tau PET positivity in the temporal meta-ROI was 88.6% for AD dementia, 46.5% for MCI, 9.5% for non-AD, and 6.1% for CU. Among Aβ+ participants with AD dementia and MCI, lower age, MMSE score, and AD-signature cortical thickness showed the strongest associations with tau PET positivity. In non-AD and CU participants, presence of Aβ was the strongest predictor of a positive tau PET scan. Conclusion: We identified several demographic, clinical, and neurobiological factors that are important to explain the variance in tau PET retention observed across the AD pathological continuum, non-AD neurodegenerative disorders, and cognitively unimpaired persons. [ABSTRACT FROM AUTHOR]

Published

2021

6. Stage-specific links between plasma neurofilament light and imaging biomarkers of Alzheimer's disease.

Author

Benedet, Andréa L, Leuzy, Antoine, Pascoal, Tharick A, Ashton, Nicholas J, Mathotaarachchi, Sulantha, Savard, Melissa, Therriault, Joseph, Kang, Min Su, Chamoun, Mira, Schöll, Michael, Zimmer, Eduardo R, Gauthier, Serge, Labbe, Aurélie, Zetterberg, Henrik, Rosa-Neto, Pedro, Blennow, Kaj, Initiative, for the Alzheimer's Disease Neuroimaging, and Alzheimer’s Disease Neuroimaging Initiative

Subjects

*ALZHEIMER'S disease, *CYTOPLASMIC filaments, *SINGLE molecules, *CEREBRAL atrophy, *MILD cognitive impairment, *CLINICAL drug trials

Abstract

Neurofilament light (NfL) is a marker of neuroaxonal injury, a prominent feature of Alzheimer's disease. It remains uncertain, however, how it relates to amyloid and tau pathology or neurodegeneration across the Alzheimer's disease continuum. The aim of this study was to investigate how plasma NfL relates to amyloid and tau PET and MRI measures of brain atrophy in participants with and without cognitive impairment. We retrospectively examined the association between plasma NfL and MRI measures of grey/white matter volumes in the Alzheimer's Disease Neuroimaging Initiative [ADNI: n = 1149; 382 cognitively unimpaired control subjects and 767 cognitively impaired participants (mild cognitive impairment n = 420, Alzheimer's disease dementia n = 347)]. Longitudinal plasma NfL was measured using single molecule array (Simoa) technology. Cross-sectional associations between plasma NfL and PET amyloid and tau measures were independently assessed in two cohorts: ADNI [n = 198; 110 cognitively unimpaired, 88 cognitively impaired (MCI n = 67, Alzheimer's disease dementia n = 21), data accessed October 2018]; and Translational Biomarkers in Aging and Dementia [TRIAD, n = 116; 74 cognitively unimpaired, 42 cognitively impaired (MCI n = 16, Alzheimer's disease dementia n = 26), data obtained November 2017 to January 2019]. Associations between plasma NfL and imaging-derived measures were examined voxel-wise using linear regression (cross-sectional) and linear mixed effect models (longitudinal). Cross-sectional analyses in both cohorts showed that plasma NfL was associated with PET findings in brain regions typically affected by Alzheimer's disease; associations were specific to amyloid PET in cognitively unimpaired and tau PET in cognitively impaired (P < 0.05). Longitudinal analyses showed that NfL levels were associated with grey/white matter volume loss; grey matter atrophy in cognitively unimpaired was specific to APOE ε4 carriers (P < 0.05). These findings suggest that plasma NfL increases in response to amyloid-related neuronal injury in preclinical stages of Alzheimer's disease, but is related to tau-mediated neurodegeneration in symptomatic patients. As such, plasma NfL may a useful measure to monitor effects in disease-modifying drug trials. [ABSTRACT FROM AUTHOR]

Published

2020

7. Bis(monoacylglycero)phosphate, a new lipid signature of endosome-derived extracellular vesicles.

Author

Rabia, Maxence, Leuzy, Valentin, Soulage, Christophe, Durand, Annie, Fourmaux, Baptiste, Errazuriz-Cerda, Elisabeth, Köffel, René, Draeger, Annette, Colosetti, Pascal, Jalabert, Audrey, Di Filippo, Mathilde, Villard-Garon, Audrey, Bergerot, Cyrille, Luquain-Costaz, Céline, Moulin, Philippe, Rome, Sophie, Delton, Isabelle, and Hullin-Matsuda, Françoise

Subjects

*EXTRACELLULAR vesicles, *LYSOSOMES, *EXOSOMES, *LYSOSOMAL storage diseases, *URINATION, *EXTRACELLULAR fluid, *LIPIDS

Abstract

Bis(monoacylglycero)phosphate (BMP), also known as lysobisphosphatidic acid (LBPA), is a phospholipid specifically enriched in the late endosome-lysosome compartment playing a crucial role for the fate of endocytosed components. Due to its presence in extracellular fluids during diseases associated with endolysosomal dysfunction, it is considered as a possible biomarker of disorders such as genetic lysosomal storage diseases and cationic amphiphilic drug-induced phospholipidosis. However, there is no true validation of this biomarker in human studies, nor a clear identification of the carrier of this endolysosome-specific lipid in biofluids. The present study demonstrates that in absence of any sign of renal failure, BMP, especially all docosahexaenoyl containing species, are significantly increased in the urine of patients treated with the antiarrhythmic drug amiodarone. Such urinary BMP increase could reflect a generalized drug-induced perturbation of the endolysosome compartment as observed in vitro with amiodarone-treated human macrophages. Noteworthy, BMP was associated with extracellular vesicles (EVs) isolated from human urines and extracellular medium of human embryonic kidney HEK293 cells and co-localizing with classical EV protein markers CD63 and ALIX. In the context of drug-induced endolysosomal dysfunction, increased BMP-rich EV release could be useful to remove excess of undigested material. This first human pilot study not only reveals BMP as a urinary biomarker of amiodarone-induced endolysosomal dysfunction, but also highlights its utility to prove the endosomal origin of EVs, also named as exosomes. This peculiar lipid already known as a canonical late endosome-lysosome marker, may be thus considered as a new lipid marker of urinary exosomes. Image 1 • Endosomal bis(monoacylglycero)phosphate BMP is detected in urinary extracellular vesicles EV. • Amiodarone-induced endosomal dysfunction increases EV secretion in human urines. • All the BMP docosahexaenoyl species increased in human urinary EV after amiodarone. • Presence of BMP in urinary EV suggests their endosomal origin as exosomes. • BMP is a new lipid marker of urinary exosomes formed from endosomal membranes. [ABSTRACT FROM AUTHOR]

Published

2020

8. Propagation of Tau Pathology: Integrating Insights From Postmortem and In Vivo Studies.

Author

Vogels, Thomas, Leuzy, Antoine, Cicognola, Claudia, Ashton, Nicholas J., Smolek, Tomas, Novak, Michal, Blennow, Kaj, Zetterberg, Henrik, Hromadka, Tomas, Zilka, Norbert, and Schöll, Michael

Subjects

*CHRONIC traumatic encephalopathy, *PROGRESSIVE supranuclear palsy, *POSITRON emission tomography, *FORENSIC pathology, *PATHOLOGY, *ALZHEIMER'S disease, *AUTOPSY

Abstract

Cellular accumulation of aggregated forms of the protein tau is a defining feature of so-called tauopathies such as Alzheimer's disease, progressive supranuclear palsy, and chronic traumatic encephalopathy. A growing body of literature suggests that conformational characteristics of tau filaments, along with regional vulnerability to tau pathology, account for the distinct histopathological morphologies, biochemical composition, and affected cell types seen across these disorders. In this review, we describe and discuss recent evidence from human postmortem and clinical biomarker studies addressing the differential vulnerability of brain areas to tau pathology, its cell-to-cell transmission, and characteristics of the different strains that tau aggregates can adopt. Cellular biosensor assays are increasingly used in human tissue to detect the earliest forms of tau pathology, before overt histopathological lesions (i.e., neurofibrillary tangles) are apparent. Animal models with localized tau expression are used to uncover the mechanisms that influence spreading of tau aggregates. Further, studies of human postmortem-derived tau filaments from different tauopathies injected in rodents have led to striking findings that recapitulate neuropathology-based staging of tau. Furthermore, the recent advent of tau positron emission tomography and novel fluid-based biomarkers render it possible to study the temporal progression of tau pathology in vivo. Ultimately, evidence from these approaches must be integrated to better understand the onset and progression of tau pathology across tauopathies. This will lead to improved methods for the detection and monitoring of disease progression and, hopefully, to the development and refinement of tau-based therapeutics. [ABSTRACT FROM AUTHOR]

Published

2020

9. Clinical impact of [18F]flutemetamol PET among memory clinic patients with an unclear diagnosis.

Author

Leuzy, Antoine, Savitcheva, Irina, Chiotis, Konstantinos, Lilja, Johan, Andersen, Pia, Bogdanovic, Nenad, Jelic, Vesna, and Nordberg, Agneta

Subjects

*DIAGNOSIS, *POSITRON emission tomography, *NEUROPSYCHOLOGICAL tests, *COGNITION disorders, *ALZHEIMER'S disease

Abstract

Purpose: To investigate the impact of amyloid PET with [18F]flutemetamol on diagnosis and treatment management in a cohort of patients attending a tertiary memory clinic in whom, despite extensive cognitive assessment including neuropsychological testing, structural imaging, CSF biomarker analysis and in some cases [18F]FDG PET, the diagnosis remained unclear. Methods: The study population consisted of 207 patients with a clinical diagnosis prior to [18F]flutemetamol PET including mild cognitive impairment (MCI; n = 131), Alzheimer's disease (AD; n = 41), non-AD (n = 10), dementia not otherwise specified (dementia NOS; n = 20) and subjective cognitive decline (SCD; n = 5). Results: Amyloid positivity was found in 53% of MCI, 68% of AD, 20% of non-AD, 20% of dementia NOS, and 60% of SCD patients. [18F]Flutemetamol PET led, overall, to a change in diagnosis in 92 of the 207 patients (44%). A high percentage of patients with a change in diagnosis was observed in the MCI group (n = 67, 51%) and in the dementia NOS group (n = 11; 55%), followed by the non-AD and AD (30% and 20%, respectively). A significant increase in cholinesterase inhibitor treatment was observed after [18F]flutemetamol PET (+218%, 34 patients before and 108 patients after). Conclusion: The present study lends support to the clinical value of amyloid PET in patients with an uncertain diagnosis in the tertiary memory clinic setting. [ABSTRACT FROM AUTHOR]

Published

2019

10. Longitudinal tau and metabolic PET imaging in relation to novel CSF tau measures in Alzheimer's disease.

Author

Leuzy, Antoine, Chiotis, Konstantinos, Lemoine, Laetitia, Saint-Aubert, Laure, Nordberg, Agneta, Cicognola, Claudia, Blennow, Kaj, Höglund, Kina, Zetterberg, Henrik, Andreasen, Niels, and Ye, Keqiang

Subjects

*ALZHEIMER'S disease, *POSITRON emission tomography, *GLUCOSE metabolism, *NEURODEGENERATION, *THREONINE

Abstract

Purpose: Studies comparing CSF and PET tau biomarkers have included only commercial CSF assays examining specific phosphorylation sites (e.g. threonine 181, P-tau181p) and mid-domain tau (i.e. total tau, T-tau). Moreover, these studies did not examine CSF tau levels in relation to cerebral glucose metabolism. We thus aimed to examine CSF tau measures, using both commercial and novel assays, in relation to [18F]THK5317 (tau) and [18F]FDG PET (glucose metabolism). Methods: Fourteen Alzheimer's disease (AD) patients (seven prodromal, seven dementia) underwent [18F]THK5317 and [18F]FDG PET studies, with follow-up performed in ten subjects (six prodromal, four dementia) after 17 months. In addition to commercial assays, novel measures capturing N-terminus+mid-domain (tau N-Mid) and C-terminally truncated (tau-368) fragments were included. Results: While the levels of all forms of CSF tau were found to be inversely associated with baseline [18F]FDG uptake, associations with baseline [18F]THK5317 uptake varied in relation to the degree of isocortical hypometabolism ([18F]FDG SUVR). Changes in the levels of the novel CSF markers tracked longitudinal changes in tracer uptake better than changes in P-tau181p and T-tau levels, and improved concordance with dichotomized regional [18F]THK5317 measures. Conclusion: Our findings suggest that neurodegeneration may modulate the relationship between CSF and PET tau biomarkers, and that, by comparison to P-tau181p and T-tau, tau-368 and tau N-Mid may better capture tau pathology and synaptic impairment. [ABSTRACT FROM AUTHOR]

Published

2019

11. Comparability of [18F]THK5317 and [11C]PIB blood flow proxy images with [18F]FDG positron emission tomography in Alzheimer’s disease.

Author

Rodriguez-Vieitez, Elena, Leuzy, Antoine, Chiotis, Konstantinos, Saint-Aubert, Laure, Wall, Anders, and Nordberg, Agneta

Abstract

For amyloid positron emission tomography tracers, the simplified reference tissue model derived ratio of influx rate in target relative to reference region (R1) has been shown to serve as a marker of brain perfusion, and, due to the strong coupling between perfusion and metabolism, as a proxy for glucose metabolism. In the present study, 11 prodromal Alzheimer’s disease and nine Alzheimer’s disease dementia patients underwent [18F]THK5317, carbon-11 Pittsburgh Compound-B ([11C]PIB), and 2-deoxy-2-[18F]fluoro-D-glucose ([18F]FDG) positron emission tomography to assess the possible use of early-phase [18F]THK5317 and R1 as proxies for brain perfusion, and thus, for glucose metabolism. Discriminative performance (prodromal vs Alzheimer’s disease dementia) of [18F]THK5317 (early-phase SUVr and R1) was compared with that of [11C]PIB (early-phase SUVr and R1) and [18F]FDG. Strong positive correlations were found between [18F]THK5317 (early-phase, R1) and [18F]FDG, particularly in frontal and temporoparietal regions. Differences in correlations between early-phase and R1 ([18F]THK5317 and [11C]PIB) and [18F]FDG, were not statistically significant, nor were differences in area under the curve values in the discriminative analysis. Our findings suggest that early-phase [18F]THK5317 and R1 provide information on brain perfusion, closely related to glucose metabolism. As such, a single positron emission tomography study with [18F]THK5317 may provide information about both tau pathology and brain perfusion in Alzheimer’s disease, with potential clinical applications. [ABSTRACT FROM AUTHOR]

Published

2017

12. Pittsburgh compound B imaging and cerebrospinal fluid amyloid-β in a multicentre European memory clinic study.

Author

Leuzy, Antoine, Chiotis, Konstantinos, Hasselbalch, Steen G., Rinne, Juha O., de Mendonça, Alexandre, Otto, Markus, Lleó, Alberto, Castelo-Branco, Miguel, Santana, Isabel, Johansson, Jarkko, Anderl-Straub, Sarah, von Arnim, Christine A. F., Beer, Ambros, Blesa, Rafael, Fortea, Juan, Herukka, Sanna-Kaisa, Portelius, Erik, Pannee, Josef, Zetterberg, Henrik, and Blennow, Kaj

Subjects

*CEREBROSPINAL fluid, *ENZYME-linked immunosorbent assay, *BIOMARKERS, *ELECTROCHEMILUMINESCENCE, *ALZHEIMER'S disease, *AMINES, *COMPARATIVE studies, *DEMENTIA, *MASS spectrometry, *RESEARCH methodology, *MEDICAL cooperation, *PEPTIDES, *RESEARCH, *THIAZOLES, *POSITRON emission tomography, *EVALUATION research

Abstract

The aim of this study was to assess the agreement between data on cerebral amyloidosis, derived using Pittsburgh compound B positron emission tomography and (i) multi-laboratory INNOTEST enzyme linked immunosorbent assay derived cerebrospinal fluid concentrations of amyloid-β42; (ii) centrally measured cerebrospinal fluid amyloid-β42 using a Meso Scale Discovery enzyme linked immunosorbent assay; and (iii) cerebrospinal fluid amyloid-β42 centrally measured using an antibody-independent mass spectrometry-based reference method. Moreover, we examined the hypothesis that discordance between amyloid biomarker measurements may be due to interindividual differences in total amyloid-β production, by using the ratio of amyloid-β42 to amyloid-β40 Our study population consisted of 243 subjects from seven centres belonging to the Biomarkers for Alzheimer's and Parkinson's Disease Initiative, and included subjects with normal cognition and patients with mild cognitive impairment, Alzheimer's disease dementia, frontotemporal dementia, and vascular dementia. All had Pittsburgh compound B positron emission tomography data, cerebrospinal fluid INNOTEST amyloid-β42 values, and cerebrospinal fluid samples available for reanalysis. Cerebrospinal fluid samples were reanalysed (amyloid-β42 and amyloid-β40) using Meso Scale Discovery electrochemiluminescence enzyme linked immunosorbent assay technology, and a novel, antibody-independent, mass spectrometry reference method. Pittsburgh compound B standardized uptake value ratio results were scaled using the Centiloid method. Concordance between Meso Scale Discovery/mass spectrometry reference measurement procedure findings and Pittsburgh compound B was high in subjects with mild cognitive impairment and Alzheimer's disease, while more variable results were observed for cognitively normal and non-Alzheimer's disease groups. Agreement between Pittsburgh compound B classification and Meso Scale Discovery/mass spectrometry reference measurement procedure findings was further improved when using amyloid-β42/40 Agreement between Pittsburgh compound B visual ratings and Centiloids was near complete. Despite improved agreement between Pittsburgh compound B and centrally analysed cerebrospinal fluid, a minority of subjects showed discordant findings. While future studies are needed, our results suggest that amyloid biomarker results may not be interchangeable in some individuals. [ABSTRACT FROM AUTHOR]

Published

2016

13. In vivo characterization of metabotropic glutamate receptor type 5 abnormalities in behavioral variant FTD.

Author

Leuzy, Antoine, Zimmer, Eduardo, Dubois, Jonathan, Pruessner, Jens, Cooperman, Cory, Soucy, Jean-Paul, Kostikov, Alexey, Schirmaccher, Esther, Désautels, René, Gauthier, Serge, and Rosa-Neto, Pedro

Subjects

*FRONTOTEMPORAL dementia, *GLUTAMATE receptors, *POSITRON emission tomography, *RADIOPHARMACEUTICALS, *NEURODEGENERATION, *DRUG bioavailability, *THERAPEUTICS

Abstract

Although the pathogenesis underlying behavioral variant frontotemporal dementia (bvFTD) has yet to be fully understood, glutamatergic abnormalities have been hypothesized to play an important role. The aim of the present study was to determine the availability of the metabotropic glutamate receptor type 5 (mGluR5) using a novel positron emission tomography (PET) radiopharmaceutical with high selectivity for mGluR5 ([C]ABP688) in a sample of bvFTD patients. In addition, we sought to determine the overlap between availability of mGluR5 and neurodegeneration, as measured using [F]FDG-PET and voxel-based morphometry (VBM). Availability of mGluR5 and glucose metabolism ([F]FDG) were measured in bvFTD ( n = 5) and cognitively normal (CN) subjects ( n = 10). [C]ABP688 binding potential maps (BP) were calculated using the cerebellum as a reference region, with [F]FDG standardized uptake ratio maps (SUV) normalized to the pons. Grey matter (GM) concentrations were determined using VBM. Voxel-based group differences were obtained using RMINC. BvFTD patients showed widespread decrements in [C]ABP688 BP throughout frontal, temporal and subcortical areas. These areas were likewise characterized by significant hypometabolism and GM loss, with overlap between reduced [C]ABP688 BP and hypometabolism superior to that for GM atrophy. Several regions were characterized only by decreased binding of [C]ABP688. The present findings represent the first in vivo report of decreased availability of mGluR5 in bvFTD. This study suggests that glutamate excitotoxicity may play a role in the pathogenesis of bvFTD and that [C]ABP688 may prove a suitable marker of glutamatergic neurotransmission in vivo. [ABSTRACT FROM AUTHOR]

Published

2016

14. Imaging β-amyloid using [F]flutemetamol positron emission tomography: from dosimetry to clinical diagnosis.

Author

Heurling, Kerstin, Leuzy, Antoine, Zimmer, Eduardo, Lubberink, Mark, and Nordberg, Agneta

Subjects

*AMYLOID, *POSITRON emission tomography, *RADIATION dosimetry, *ALZHEIMER'S disease diagnosis, *NEURODEGENERATION, *LIGANDS (Biochemistry), *MILD cognitive impairment

Abstract

In Alzheimer's disease (AD), the deposition of β-amyloid (Aβ) is hypothesized to result in a series of secondary neurodegenerative processes, leading ultimately to synaptic dysfunction and neuronal loss. Since the advent of the first Aβ-specific positron emission tomography (PET) ligand, C-Pittsburgh compound B ([C]PIB), several F ligands have been developed that circumvent the limitations of [C]PIB tied to its short half-life. To date, three such compounds have been approved for clinical use by the US and European regulatory bodies, including [F]AV-45 ([F]florbetapir; Amyvid™), [F]-BAY94-9172 ([F]florbetaben; Neuraceq™) and [F]3′-F-PIB ([F]flutemetamol; Vizamyl™). The present review aims to summarize and discuss the currently available knowledge on [F]flutemetamol PET. As the F analogue of [C]PIB, [F]flutemetamol may be of use in the differentiation of AD from related neurodegenerative disorders and may help with subject selection and measurement of target engagement in the context of clinical trials testing anti-amyloid therapeutics. We will also discuss its potential use in non-AD amyloidopathies. [ABSTRACT FROM AUTHOR]

Published

2016

15. Concordance and Diagnostic Accuracy of [11C]PIB PET and Cerebrospinal Fluid Biomarkers in a Sample of Patients with Mild Cognitive Impairment and Alzheimer's Disease.

Author

Leuzy, Antoine, Carter, Stephen F., Chiotis, Konstantinos, Almkvist, Ove, Wall, Anders, and Nordberg, Agneta

Subjects

*MILD cognitive impairment, *CEREBROSPINAL fluid, *ALZHEIMER'S disease research, *AMYLOID beta-protein, *BIOMARKERS, *TOMOGRAPHY, *DIAGNOSIS

Abstract

Background: Alzheimer's disease (AD) pathology can be quantified in vivo using cerebrospinal fluid (CSF) levels of amyloid-β1-42 (Aβ1-42), total-tau (t-tau), and phosphorylated tau (p-tau181p), as well as with positron emission tomography (PET) using [11C]Pittsburgh compound-B ([11C]PIB). Studies assessing concordance between these measures, however, have provided conflicting results. Moreover, it has been proposed that [11C]PIB PET may be of greater clinical utility in terms of identifying patients with mild cognitive impairment (MCI) who will progress to the dementia phase of AD. Objective: To determine concordance and classification accuracy of CSF biomarkers and [11C]PIB PET in a cohort of patients with MCI and AD. Methods: 68 patients (MCI, n = 33; AD, n = 35) underwent [11C]PIB PET and CSF sampling. Cutoffs of >1.41 ([11C]PIB), <450 pg/mL-and a more lenient cutoff of 550 pg/mL-(Aβ1-42), <6.5 (Aβ1-42/p-tau181p), and 1.14 (Aβ1-42/t-tau), were used to determine concordance. Logistic regression was used to determine classification accuracy with respect to stable MCI (sMCI) versus MCI who progressed to AD (pMCI). Results: Concordance between [11C]PIB and Aβ1-42 was highest for sMCI (67%), followed by AD (60%) and pMCI (33%). Agreement was increased across groups using Aβ1-42 <550 pg/mL, or Aβ1-42 to tau ratios. Logistic regression showed that classification accuracy of [11C]PIB, between sMCI and pMCI, was superior to Aβ1-42 (73% versus 58%), Aβ1-42/t-tau (63%), and Aβ1-42/p-tau181p (65%). Conclusion: In the present study, [11C]PIB proved a better predictor of progression to AD in patients with MCI, relative to CSF measures of Aβ1-42 or Aβ1-42/tau. Discordance between PET and CSF markers for Aβ1-42 suggests they cannot be used interchangeably, as is currently the case. [ABSTRACT FROM AUTHOR]

Published

2015

16. Concordance and Diagnostic Accuracy of [11C]PIB PET and Cerebrospinal Fluid Biomarkers in a Sample of Patients with Mild Cognitive Impairment and Alzheimer's Disease.

Author

Leuzy, Antoine, Carter, Stephen F, Chiotis, Konstantinos, Almkvist, Ove, Wall, Anders, and Nordberg, Agneta

Abstract

Background: Alzheimer's disease (AD) pathology can be quantified in vivo using cerebrospinal fluid (CSF) levels of amyloid-β1-42 (Aβ1-42), total-tau (t-tau), and phosphorylated tau (p-tau181p), as well as with positron emission tomography (PET) using [(11)C]Pittsburgh compound-B ([(11)C]PIB). Studies assessing concordance between these measures, however, have provided conflicting results. Moreover, it has been proposed that [(11)C]PIB PET may be of greater clinical utility in terms of identifying patients with mild cognitive impairment (MCI) who will progress to the dementia phase of AD.Objective: To determine concordance and classification accuracy of CSF biomarkers and [(11)C]PIB PET in a cohort of patients with MCI and AD.Methods: 68 patients (MCI, n = 33; AD, n = 35) underwent [(11)C]PIB PET and CSF sampling. Cutoffs of >1.41 ([(11)C]PIB), <450 pg/mL-and a more lenient cutoff of 550 pg/mL-(Aβ1-42), <6.5 (Aβ1-42/p-tau181p), and 1.14 (Aβ1-42/t-tau), were used to determine concordance. Logistic regression was used to determine classification accuracy with respect to stable MCI (sMCI) versus MCI who progressed to AD (pMCI).Results: Concordance between [(11)C]PIB and Aβ1-42 was highest for sMCI (67%), followed by AD (60%) and pMCI (33%). Agreement was increased across groups using Aβ1-42 <550 pg/mL, or Aβ1-42 to tau ratios. Logistic regression showed that classification accuracy of [(11)C]PIB, between sMCI and pMCI, was superior to Aβ1-42 (73% versus 58%), Aβ1-42/t-tau (63%), and Aβ1-42/p-tau181p (65%).Conclusion: In the present study, [(11)C]PIB proved a better predictor of progression to AD in patients with MCI, relative to CSF measures of Aβ1-42 or Aβ1-42/tau. Discordance between PET and CSF markers for Aβ1-42 suggests they cannot be used interchangeably, as is currently the case. [ABSTRACT FROM AUTHOR]

Published

2015

17. Use of amyloid PET across the spectrum of Alzheimer's disease: clinical utility and associated ethical issues.

Author

Leuzy, Antoine, Zimmer, Eduardo Rigon, Heurling, Kerstin, Rosa-Neto, Pedro, and Gauthier, Serge

Subjects

*POSITRON emission tomography, *ALZHEIMER'S disease, *AMYLOID, *DIAGNOSIS, *GLYCOPROTEINS

Abstract

Recent advances have made possible the in vivo detection of beta-amyloid (Aβ) pathology using positron emission tomography. While the gold standard for amyloid imaging, carbon-11 labeled Pittsburgh compound B is increasingly being replaced by fluorine-18 labeled radiopharmaceuticals, with three already approved for clinical use by US and European regulatory bodies. Appropriate use criteria proposed by an amyloid imaging taskforce convened by the Alzheimer's Association and the Society of Nuclear Medicine and Molecular Imaging recommend restricting use of this technology to the evaluation of patients with mild cognitive impairment or atypical dementia syndromes. While use among asymptomatic individuals is currently viewed as inappropriate due prognostic uncertainty, elevated levels of brain Aβ among asymptomatic individuals may represent preclinical Alzheimer's disease. Amyloid imaging is likewise expected to play a role in the design of clinical trials. Though preliminary results suggest amyloid imaging to possess clinical utility and cost-effectiveness, both domains have yet to be assessed systematically. As the field moves toward adoption of a pro-disclosure stance for amyloid imaging findings, it is imperative that a broad range of stakeholders be involved to ensure the appropriateness of emerging policies and protocols. [ABSTRACT FROM AUTHOR]

Published

2014

18. Diagnosis and management of Alzheimer's disease: Past, present and future ethical issues.

Author

Gauthier, S., Leuzy, A., Racine, E., and Rosa-Neto, P.

Subjects

*ALZHEIMER'S disease diagnosis, *ALZHEIMER'S disease treatment, *BIOMARKERS, *CARE of people, *ETHICS, *EARLY diagnosis

Abstract

Highlights: [•] Ethical issues associated with the care of persons with Alzheimer's disease are numerous. [•] Ethical issues associated with the care of persons with Alzheimer's disease are differ between presymptomatic, early symptomatic and late stages of disease. [•] New challenges are emerging with very early diagnosis requiring biomarkers and potentially expensive therapies. [•] Interested parties need to develop a structured approach to the future treatment of Alzheimer's disease. [ABSTRACT FROM AUTHOR]

Published

2013

19. Revising the Diagnostic Criteria for Alzheimer's Disease: The Use of Biomarkers and Attendant Ethical Implications.

Author

Leuzy, Antoine, Rosa-Neto, Pedro, and Gauthier, Serge

Subjects

*ALZHEIMER'S disease diagnosis, *ALZHEIMER'S disease treatment, *PATHOLOGICAL physiology, *BIOMARKERS, *TREATMENT of dementia, *DISEASE prevalence, *NEUROBIOLOGY

Abstract

"Alzheimer's disease (AD) accounts for approximately 70 percent of dementia cases and is characterized by the need for specialized, high cost, long-term care. It is estimated that by the year 2050, AD will affect 13.5 million individuals within the US alone, a prevalence rate representing 10% of that predicted at the global level. As such, AD stands as one of the most important health challenges of the 21st century. While initially viewed as a distinct clinicopathological entity -- with the attendant implications of synonymity between AD pathology and the clinical symptoms of AD -- advances in the neurobiology of AD have led to a revised conceptualization of AD in which the underlying pathophysiology is thought to precede the clinical diagnosis of AD by up to a decade. This has led to a growing consensus that the predementia phase of AD may represent a therapeutic window of opportunity -- a period during which disease modifying drugs may prove effective -- and has resulted in: 1) an increasing shift toward the use of biomarkers -- measures that allow for in vivo detection of AD pathophysiology; and 2) the concept of early disease modifying interventions as a strategy to prevent or delay dementia onset. Collectively, these elements have found expression in the recent revisions to the diagnostic criteria for AD, namely those advanced by the National Institute of Aging and Alzheimer's Association workgroups. While these developments signal progress in the fight against AD, they likewise bring to the fore ethical implications that merit careful consideration. These are the potential impact of a diagnosis of AD in its predementia stages and the implications of the new criteria on practicing physicians, those working in memory clinics, and society as a whole." [ABSTRACT FROM AUTHOR]

Published

2013

20. How Can We Improve Transfer of Outcomes from Randomized Clinical Trials to Clinical Practice with Disease-Modifying Drugs in Alzheimer's Disease?

Author

Gauthier, S., Leuzy, A., and Rosa-Neto, P.

Subjects

*ALZHEIMER'S disease treatment, *TREATMENT effectiveness, *CLINICAL trials, *MEDICAL practice, *DISEASE progression, *DRUG side effects

Abstract

Background: Randomized clinical trials (RCTs) for putative disease-modifying drugs in Alzheimer's disease (AD) are using cognitive outcomes, such as the Alzheimer's Disease Assessment Scale - cognitive subscale, activities of daily living scales, such as the Alzheimer's Disease Cooperative Study Activities of Daily Living, and time from mild cognitive impairment to AD dementia. Objective: It was the aim of this study to build clinically relevant outcomes for future use in clinical practice into RCT designs and help third-party payers to measure benefit. Methods: We used a literature review for analysis. Results: The Clinical Dementia Rating Scale Sum of Boxes (CDR-SB) appears to be the most reliable primary outcome for RCT at different stages of AD, with the Relevant Outcome Scale for Alzheimer's Disease (ROSA) as a suitable alternative. The importance of current AD biomarkers vis-à- vis determination of efficacy of disease-modifying drugs has yet to be established; however, it is likely that at least one amyloid-specific test will be required prior to treatment with a drug acting predominantly on β-amyloid (Aβ42). Furthermore, serial MRI may be required to monitor adverse side effects associated with such drugs. Conclusions: Global clinical scales such as CDR-SB and ROSA should be considered for use with treatments aiming at slowing disease progression. © 2013 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2014

21. Compensating for choroid plexus based off-target signal in the hippocampus using 18F-flortaucipir PET.

Author

Pawlik, Daria, Leuzy, Antoine, Strandberg, Olof, and Smith, Ruben

Subjects

*CHOROID plexus, *HIPPOCAMPUS (Brain), *ALZHEIMER'S disease

Abstract

Purpose: The hippocampus is affected by tau pathology early in Alzheimer's disease (AD) development. Accurate quantification of hippocampal tau signal using the tau-PET tracer 18F-flortaucipir is complicated, however, by off-target binding in the adjacent choroid plexus. We here present a new method for compensating for this off-target choroid plexus signal. Methods: As off-target binding in the choroid plexus is known to be higher using 18F-flortaucipir compared to 18F-RO948, we created a binary hippocampal mask in template space where 18F-flortaucipir signal was higher than 18F-RO948, using data from 30 patients that underwent both 18F-flortaucipir and 18F-RO948 PET. This mask, presumably representing hippocampal voxels affected by off-target binding from the choroid plexus, was then converted to native space and applied as an exclusion mask to 145 patients across the AD-spectrum scanned with 18F-flortaucipir. As an alternative approach exclusion masks were generated by expanding the choroid plexus ROI in native space. Results were analysed both without and with partial volume error correction (non-PVEc/PVEc). Results: Unmasked hippocampal standardized uptake value ratios (SUVR) were significantly correlated to choroid plexus SUVRs using both non-PVEc (p < 0.001, r = 0.28) and PVEc data (p < 0.05, r = 0.18). After applying the mask, however, these correlations disappeared. The diagnostic accuracy in separating cognitively impaired (CI) from cognitively unimpaired (CU) subjects improved after masking, from an AUC of 0.792 (95% C.I.,0.715–0.869) to 0.837 (95% C.I.,0.768–0.906) for non-PVEc data (p < 0.001), and from 0.798 (95% C.I.,0.722–0.873) to 0.834 (95% C.I.,0.766–0.903) for PVEc data (p < 0.001). The correlations to memory improved significantly for MMSE for unmasked vs. masked data both without (r = −0.440 vs. r = −0.499, p < 0.001) and with (r = −0.454 vs. r = −0.503, p < 0.001) PVEc. Similar results were found using the ADAS-Cog Delayed Word Recall test. Conclusion: Choroid plexus off-target binding interferes with the estimation of true hippocampal retention using 18F-flortaucipir PET. Using a mask to correct for this off-target signal, we improved the diagnostic accuracy of 18F-flortaucipir in the hippocampus and the correlation between 18F-flortaucipir hippocampal SUVR and cognitive measures. [ABSTRACT FROM AUTHOR]

Published

2020

22. Association of in vivo retention of [18f] flortaucipir pet with tau neuropathology in corresponding brain regions.

Author

Freiburghaus, Tove, Pawlik, Daria, Oliveira Hauer, Kevin, Ossenkoppele, Rik, Strandberg, Olof, Leuzy, Antoine, Rittmo, Jonathan, Tremblay, Cécilia, Serrano, Geidy E., Pontecorvo, Michael J., Beach, Thomas G., Smith, Ruben, and Hansson, Oskar

Subjects

*AMYLOID plaque, *ALZHEIMER'S disease, *AUTOPSY, *POSITRON emission tomography, *TAUOPATHIES

Abstract

[18F]Flortaucipir is an FDA-approved tau-PET tracer that is increasingly utilized in clinical settings for the diagnosis of Alzheimer's disease. Still, a large-scale comparison of the in vivo PET uptake to quantitative post-mortem tau pathology and to other co-pathologies is lacking. Here, we examined the correlation between in vivo [18F]flortaucipir PET uptake and quantitative post-mortem tau pathology in corresponding brain regions from the AVID A16 end-of-life study (n = 63). All participants underwent [18F]flortaucipir PET scans prior to death, followed by a detailed post-mortem neuropathological examination using AT8 (tau) immunohistochemistry. Correlations between [18F]flortaucipir standardized uptake value ratios (SUVRs) and AT8 immunohistochemistry were assessed across 18 regions-of-interest (ROIs). To assess [18F]flortaucipir specificity and level of detection for tau pathology, correlations between [18F]flortaucipir SUVR and neuritic plaque score and TDP-43 stage were also computed and retention was further assessed in individuals with possible primary age-related tauopathy (PART), defined as Thal phase ≤ 2 and Braak stage I–IV. We found modest-to-strong correlations between in vivo [18F]flortaucipir SUVR and post-mortem tau pathology density in corresponding brain regions in all neocortical regions analyzed (rho-range = 0.61–0.79, p < 0.0001 for all). The detection threshold of [18F]flortaucipir PET was determined to be 0.85% of surface area affected by tau pathology in a temporal meta-ROI, and 0.15% in a larger cortical meta-ROI. No significant associations were found between [18F]flortaucipir SUVRs and post-mortem tau pathology in individuals with possible PART. Further, there was no correlation observed between [18F]flortaucipir and level of amyloid-β neuritic plaque load (rho-range = – 0.16–0.12; p = 0.48–0.61) or TDP-43 stage (rho-range = – 0.10 to – 0.30; p = 0.18–0.65). In conclusion, our in vivo vs post-mortem study shows that the in vivo [18F]flortaucipir PET signal primarily reflects tau pathology, also at relatively low densities of tau proteinopathy, and does not bind substantially to tau neurites in neuritic plaques or in individuals with PART. [ABSTRACT FROM AUTHOR]

Published

2024

23. 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

24. Increased plasma neurofilament light chain concentration correlates with severity of post-mortem neurofibrillary tangle pathology and neurodegeneration.

Author

Ashton, Nicholas J., Leuzy, Antoine, Lim, Yau Mun, Troakes, Claire, Hortobágyi, Tibor, Höglund, Kina, Aarsland, Dag, Lovestone, Simon, Schöll, Michael, Blennow, Kaj, Zetterberg, Henrik, and Hye, Abdul

Subjects

*ALZHEIMER'S disease, *CYTOPLASMIC filaments, *NEURODEGENERATION

Abstract

Alzheimer's disease (AD) is pathologically characterized by the accumulation of amyloid-β (Aβ) plaques, neurofibrillary tangles and widespread neuronal loss in the brain. In recent years, blood biomarkers have emerged as a realistic prospect to highlight accumulating pathology for secondary prevention trials. Neurofilament light chain (NfL), a marker of axonal degeneration, is robustly elevated in the blood of many neurological and neurodegenerative conditions, including AD. A strong relationship with cerebrospinal fluid (CSF) NfL suggests that these biomarker modalities reflect the same pathological process. Yet, the connection between blood NfL and brain tissue pathology has not been directly compared. In this study, longitudinal plasma NfL from cognitively healthy controls (n = 12) and AD participants (n = 57) were quantified by the Simoa platform. On reaching post-mortem, neuropathological assessment was performed on all participants, with additional frozen and paraffin-embedded tissue acquired from 26 participants for further biochemical (Aβ1–42, Aβ1–40, tau) and histological (NfL) evaluation. Plasma NfL concentrations were significantly increased in AD and correlated with cognitive decline, independent of age. Retrospective stratification based on Braak staging revealed that baseline plasma NfL concentrations were associated with higher neurofibrillary tangle pathology at post-mortem. Longitudinal increases in plasma NfL were observed in all Braak groupings; a significant negative association, however, was found between plasma NfL at time point 1 and both its rate of change and annual percentage increase. Immunohistochemical evaluation of NfL in the medial temporal gyrus (MTG) demonstrated an inverse relationship between Braak stages and NfL staining. Importantly, a significant negative correlation was found between the plasma NfL measurement closest to death and the level of NfL staining in the MTG at post-mortem. For the first time, we demonstrate that plasma NfL associates with the severity of neurofibrillary tangle pathology and neurodegeneration in the post-mortem brain. [ABSTRACT FROM AUTHOR]

Published

2019

25. Head-to-head comparison of tau positron emission tomography tracers [18F]flortaucipir and [18F]RO948.

Author

Smith, Ruben, Schöll, Michael, Leuzy, Antoine, Jögi, Jonas, Ohlsson, Tomas, Strandberg, Olof, and Hansson, Oskar

Subjects

*POSITRON emission tomography, *NEUROFIBRILLARY tangles, *AMNESTIC mild cognitive impairment, *ENTORHINAL cortex, *CHOROID plexus, *ALZHEIMER'S disease

Abstract

Purpose: [18F]flortaucipir binds to paired helical filament tau and accurately identifies tau in Alzheimer's disease (AD). However, "off-target" binding interferes with the quantification of [18F]flortaucipir in several brain regions. Recently, other tau PET tracers have been developed. Here, we compare [18F]flortaucipir with the novel tau tracer [18F]RO948 head-to-head in vivo. Methods: We included 18 participants with AD, three with amyloid-β-positive amnestic mild cognitive impairment, and four healthy controls. All underwent [18F]flortaucipir (80–100 min) and [18F]RO948 (70–90) PET scans within approximately 1 month. Four study participants underwent 0–100-min dynamic scanning. Standardized uptake value ratios (SUVRs) were created using an inferior cerebellar reference region. Results: Neocortical tracer retention was highly comparable using both SUVR and distribution volume ratio-1 values obtained from dynamic scans. However, [18F]RO948 retention was significantly higher in the entorhinal cortex and lower in the basal ganglia, thalamus, and choroid plexus compared with [18F]flortaucipir. Increased off-target binding was observed with age for both tracers. Several cases exhibited strong [18F]RO948 retention in the skull/meninges. This extra-cerebral signal, however, did not affect diagnostic accuracy and remained relatively unchanged when re-examining a subsample after 1 year. Kinetic modeling showed an increase in [18F]flortaucipir SUVR over the scanning interval, compared with a plateau for [18F]RO948. Conclusion: [18F]RO948 and [18F]flortaucipir bound comparably in neocortical regions, but [18F]RO948 showed higher retention in the medial temporal lobe and lower intracerebral "off-target" binding. Time-dependent bias of SUVR estimates may prove less of a factor with [18F]RO948, compared with previous tau ligands. [ABSTRACT FROM AUTHOR]

Published

2020

26. Synaptic vesicle protein 2A as a potential biomarker in synaptopathies.

Author

Heurling, Kerstin, Ashton, Nicholas J., Leuzy, Antoine, Zimmer, Eduardo R., Blennow, Kaj, Zetterberg, Henrik, Eriksson, Jonas, Lubberink, Mark, and Schöll, Michael

Subjects

*SYNAPTIC vesicles, *POSITRON emission tomography, *PATHOLOGY, *MENTAL illness, *NEURODEGENERATION

Abstract

Measuring synaptic density in vivo using positron emission tomography (PET) imaging-based biomarkers targeting the synaptic vesicle protein 2A (SV2A) has received much attention recently due to its potential research and clinical applications in synaptopathies, including neurodegenerative and psychiatric diseases. Fluid-based biomarkers in proteinopathies have previously been suggested to provide information on pathology and disease status that is complementary to PET-based measures, and the same can be hypothesized with respect to SV2A. This review provides an overview of the current state of SV2A PET imaging as a biomarker of synaptic density, the potential role of fluid-based biomarkers for SV2A, and related future perspectives. • SV2A protein is expressed in synaptic vesicles, crucial for neuronal communication. • Synaptopathies are disorders showing synaptic function and density alterations. • PET can be used to measure alterations of SV2A. • Fluid based biomarkers of SV2A holds promise as a state marker of synapthopathies. [ABSTRACT FROM AUTHOR]

Published

2019

27. Comparison of Early-Phase (S)-[18F]THK5117 and [11C]PIB PET imaging to assess brain perfusion in Alzheimer’s disease.

Author

Rodriguez-Vieitez, Elena, Leuzy, Antoine, Chiotis, Konstantinos, Saint-Aubert, Laure, and Nordberg, Agneta

Subjects

*ALZHEIMER'S disease diagnosis, *PERFUSION, *POSITRON emission tomography, *QUINOLINE derivatives, *COMPARATIVE studies

Published

2016

28. Improved concordance between [11C]PIB PET and CSF Aβ42 using Aβ42/Aβ40: findings from a multicentre European memory clinic population.

Author

Leuzy, Antoine, Chiotis, Konstantinos, Pannee, Josef, Hasselbalch, Steen, Rinne, Juha, Castelo-Branco, Miguel, Mendonca, Alexandre, Santana, Isabel, Bisa, Alberto Lléo, Johansson, Jarkko, Otto, Markus, Portelius, Erik, Zetterberg, Henrik, Blennow, Kaj, and Nordberg, Agneta

Subjects

*CEREBROSPINAL fluid, *POSITRON emission tomography, *AGE factors in memory, *NEUROBIOLOGY, *THIOFLAVINS

Published

2016

29. Tracking neuroinflammation in Alzheimer's disease: the role of positron emission tomography imaging.

Author

Zimmer, Eduardo Rigon, Leuzy, Antoine, Benedet, Andréa Lessa, Breitner, John, Gauthier, Serge, and Rosa-Neto, Pedro

Abstract

Alzheimer's disease (AD) has been reconceptualized as a dynamic pathophysiological process, where the accumulation of amyloid-beta (Aβ) is thought to trigger a cascade of neurodegenerative events resulting in cognitive impairment and, eventually, dementia. In addition to Aβ pathology, various lines of research have implicated neuroinflammation as an important participant in AD pathophysiology. Currently, neuroinflammation can be measured in vivo using positron emission tomography (PET) with ligands targeting diverse biological processes such as microglial activation, reactive astrocytes and phospholipase A2 activity. In terms of therapeutic strategies, despite a strong rationale and epidemiological studies suggesting that the use of non-steroidal anti-inflammatory drugs (NSAIDs) may reduce the prevalence of AD, clinical trials conducted to date have proven inconclusive. In this respect, it has been hypothesized that NSAIDs may only prove protective if administered early on in the disease course, prior to the accumulation of significant AD pathology. In order to test various hypotheses pertaining to the exact role of neuroinflammation in AD, studies in asymptomatic carriers of mutations deterministic for early-onset familial AD may prove of use. In this respect, PET ligands for neuroinflammation may act as surrogate markers of disease progression, allowing for the development of more integrative models of AD, as well as for the measuring of target engagement in the context of clinical trials using NSAIDs. In this review, we address the biological basis of neuroinflammatory changes in AD, underscore therapeutic strategies using anti-inflammatory compounds, and shed light on the possibility of tracking neuroinflammation in vivo using PET imaging ligands. [ABSTRACT FROM AUTHOR]

Published

2014

30. Phospho-tau with subthreshold tau-PET predicts increased tau accumulation rates in amyloid-positive individuals.

Author

Groot, Colin, Smith, Ruben, Stomrud, Erik, Binette, Alexa Pichet, Leuzy, Antoine, Wuestefeld, Anika, Wisse, Laura E M, Palmqvist, Sebastian, Mattsson-Carlgren, Niklas, Janelidze, Shorena, Strandberg, Olof, Ossenkoppele, Rik, and Hansson, Oskar

Subjects

*TAU proteins, *CHRONIC traumatic encephalopathy, *ALZHEIMER'S disease, *MILD cognitive impairment, *CEREBRAL cortical thinning, *TEMPORAL lobe

Abstract

Different tau biomarkers become abnormal at different stages of Alzheimer's disease, with CSF phospho-tau typically becoming elevated at subthreshold levels of tau-PET binding. To capitalize on the temporal order of tau biomarker-abnormality and capture the earliest changes of tau accumulation, we implemented an observational study design to examine longitudinal changes in tau-PET, cortical thickness and cognitive decline in amyloid-β-positive individuals with elevated CSF p-tau levels (P+) but subthreshold Tau-PET retention (T−). To this end, individuals without dementia (i.e. cognitively unimpaired or mild cognitive impairment, n = 231) were selected from the BioFINDER-2 study. Amyloid-β-positive (A+) individuals were categorized into biomarker groups based on cut-offs for abnormal CSF p-tau217 and 18F-RO948 (Tau) PET, yielding groups of tau-concordant-negative (A+P−T−; n = 30), tau-discordant (i.e. A+P+T−; n = 48) and tau-concordant-positive (A+P+T+; n = 18) individuals. In addition, 135 amyloid-β-negative, tau-negative, cognitively unimpaired individuals served as controls. Differences in annual change in regional tau-PET, cortical thickness and cognition between the groups were assessed using general linear models, adjusted for age, sex, clinical diagnosis and (for cognitive measures only) education. Mean follow-up time was ∼2 years. Longitudinal increase in tau-PET was faster in the A+P+T− group than in the control and A+P−T− groups across medial temporal and neocortical regions, with the highest accumulation rates in the medial temporal lobe. The A+P+T− group showed a slower rate of increase in tau-PET compared to the A+P+T+ group, primarily in neocortical regions. We did not detect differences in yearly change in cortical thickness or in cognitive decline between the A+P+T− and A+P−T− groups. The A+P+T+ group, however, showed faster cognitive decline compared to all other groups. Altogether, these findings suggest that the A+P+T− biomarker profile in persons without dementia is associated with an isolated effect on increased tau-PET accumulation rates but not on cortical thinning and cognitive decline. While this suggests that the tau-discordant biomarker profile is not strongly associated with short-term clinical decline, this group does represent an interesting population for monitoring the effects of interventions with disease-modifying agents on tau accumulation in early Alzheimer's disease, and for examining the emergence of tau aggregates in Alzheimer's disease. Further, we suggest updating the AT(N) criteria for Alzheimer's disease biomarker classification to APT(N). [ABSTRACT FROM AUTHOR]

Published

2023

31. Performance of [18F]RO948 PET, MRI and CSF neurofilament light in the differential diagnosis of progressive supranuclear palsy.

Author

Oliveira Hauer, Kevin, Pawlik, Daria, Leuzy, Antoine, Janelidze, Shorena, Hall, Sara, Hansson, Oskar, and Smith, Ruben

Subjects

*PROGRESSIVE supranuclear palsy, *DIFFERENTIAL diagnosis, *CYTOPLASMIC filaments, *RECEIVER operating characteristic curves, *GLOBUS pallidus, *MAGNETIC resonance imaging

Abstract

Introduction: The diagnosis of progressive supranuclear palsy (PSP) is often challenging since PSP may clinically resemble other neurodegenerative disorders. Recently, the tau PET tracer [18F]RO948, a potential new biomarker for PSP, was developed. The aim of this study was to determine the ability of three different biomarkers, including [18F]RO948 PET, to distinguish PSP patients from healthy controls and from patients with α-synucleinopathies.Methods: Patients with PSP (n = 23), α-synucleinopathies (n = 47) and healthy controls (n = 61) were included from the BioFINDER-2 study. [18F]RO948 standardized uptake value ratios (SUVR), magnetic resonance imaging midbrain/pons ratio, and cerebrospinal fluid neurofilament light (NfL) levels were compared between diagnostic groups individually and in combination.Results: [18F]RO948 PET SUVR in the globus pallidus, NfL, and midbrain/pons area ratios were all able to differentiate PSP patients from controls and from patients with α-synucleinopathies ([18F]RO948 [mean ± SD]: controls 1.24 ± 0.22; PSP 1.47 ± 0.4; PD 1.18 ± 0.2; DLB 1.25 ± 0.24, p < 0.05), (NfL pg/mL [mean ± SD]: controls 1055 ± 569; PSP 2197 ± 1010; PD 1038 ± 416; DLB 1548 ± 687, p < 0.001) and (midbrain/pons ratio [mean ± SD]: controls 0.46 ± 0.07; PSP 0.34 ± 0.09; PD 0.43 ± 0.06; DLB 0.40 ± 0.07, p < 0.01). Receiver operating characteristic (ROC) analyses indicated that combining the three biomarkers resulted in the highest area under the ROC values (0.94 [0.88-1.00]) for separating controls from PSP and (0.92 [0.85-0.99]) for separating PSP from α-synucleinopathies.Conclusions: All studied biomarkers could individually separate PSP from controls and α-synucleinopathies patients at a group level. The optimal prediction models included NfL and midbrain/pons ratio for separating controls from PSP and all three biomarkers for separating PSP from α-synucleinopathies. [ABSTRACT FROM AUTHOR]

Published

2023

32. Imaging in vivo glutamate fluctuations with [11C]ABP688: a GLT-1 challenge with ceftriaxone.

Author

R Zimmer, Eduardo, Parent, Maxime J, Leuzy, Antoine, Aliaga, Antonio, Aliaga, Arturo, Moquin, Luc, S Schirrmacher, Esther, Soucy, Jean-Paul, Skelin, Ivan, Gratton, Alain, Gauthier, Serge, and Rosa-Neto, Pedro

Subjects

*GLUTAMATE receptors, *CEFTRIAXONE, *BRAIN imaging, *POSITRON emission tomography, *MICRODIALYSIS, *BINDING sites, *NEUROBEHAVIORAL disorders, *LABORATORY rats

Abstract

Molecular imaging offers unprecedented opportunities for investigating dynamic changes underlying neuropsychiatric conditions. Here, we evaluated whether [11C]ABP688, a positron emission tomography (PET) ligand that binds to the allosteric site of the metabotropic glutamate receptor type 5 (mGluR5), is sensitive to glutamate fluctuations after a pharmacological challenge. For this, we used ceftriaxone (CEF) administration in rats, an activator of the GLT-1 transporter (EAAT2), which is known to decrease extracellular levels of glutamate. MicroPET [11C]ABP688 dynamic acquisitions were conducted in rats after a venous injection of either saline (baseline) or CEF 200 mg/kg (challenge). Binding potentials (BPND) were obtained using the simplified reference tissue method. Between-condition statistical parametric maps indicating brain regions showing the highest CEF effects guided placement of microdialysis probes for subsequent assessment of extracellular levels of glutamate. The CEF administration increased [11C]ABP688 BPND in the thalamic ventral anterior (VA) nucleus bilaterally. Subsequent microdialysis assessment revealed declines in extracellular glutamate concentrations in the VA. The present results support the concept that availability of mGluR5 allosteric binding sites is sensitive to extracellular concentrations of glutamate. This interesting property of mGluR5 allosteric binding sites has potential applications for assessing the role of glutamate in the pathogenesis of neuropsychiatric conditions. [ABSTRACT FROM AUTHOR]

Published

2015

33. Correction to: The Strategic Biomarker Roadmap for the validation of Alzheimer's diagnostic biomarkers: methodological update.

Author

Boccardi, Marina, Dodich, Alessandra, Albanese, Emiliano, Gayet-Ageron, Angèle, Festari, Cristina, Ashton, Nicholas J., Bischof, Gérard N., Chiotis, Konstantinos, Leuzy, Antoine, Wolters, Emma E., Walter, Martin, Rabinovici, Gil D., Carrillo, Maria, Drzezga, Alexander, Hansson, Oskar, Nordberg, Agneta, Ossenkoppele, Rik, Villemagne, Victor L., Winblad, Bengt, and Frisoni, Giovanni

Subjects

*CANCER-related mortality, *MILD cognitive impairment, *ALZHEIMER'S disease

Published

2021

34. The strategic biomarker roadmap for the validation of Alzheimer's diagnostic biomarkers: methodological update.

Author

Boccardi, Marina, Dodich, Alessandra, Albanese, Emiliano, Gayet-Ageron, Angèle, Festari, Cristina, Ashton, Nicholas J., Bischof, Gérard N., Chiotis, Konstantinos, Leuzy, Antoine, Wolters, Emma E., Walter, Martin A., Rabinovici, Gil D., Carrillo, Maria, Drzezga, Alexander, Hansson, Oskar, Nordberg, Agneta, Ossenkoppele, Rik, Villemagne, Victor L., Winblad, Bengt, and Frisoni, Giovanni B.

Subjects

*BIOMARKERS, *BIOLOGICAL tags, *MEDICAL research, *ALZHEIMER'S disease, *KNOWLEDGE gap theory, *DATA extraction

Abstract

Background: The 2017 Alzheimer's disease (AD) Strategic Biomarker Roadmap (SBR) structured the validation of AD diagnostic biomarkers into 5 phases, systematically assessing analytical validity (Phases 1–2), clinical validity (Phases 3–4), and clinical utility (Phase 5) through primary and secondary Aims. This framework allows to map knowledge gaps and research priorities, accelerating the route towards clinical implementation. Within an initiative aimed to assess the development of biomarkers of tau pathology, we revised this methodology consistently with progress in AD research. Methods: We critically appraised the adequacy of the 2017 Biomarker Roadmap within current diagnostic frameworks, discussed updates at a workshop convening the Alzheimer's Association and 8 leading AD biomarker research groups, and detailed the methods to allow consistent assessment of aims achievement for tau and other AD diagnostic biomarkers. Results: The 2020 update applies to all AD diagnostic biomarkers. In Phases 2–3, we admitted a greater variety of study designs (e.g., cross-sectional in addition to longitudinal) and reference standards (e.g., biomarker confirmation in addition to clinical progression) based on construct (in addition to criterion) validity. We structured a systematic data extraction to enable transparent and formal evidence assessment procedures. Finally, we have clarified issues that need to be addressed to generate data eligible to evidence-to-decision procedures. Discussion: This revision allows for more versatile and precise assessment of existing evidence, keeps up with theoretical developments, and helps clinical researchers in producing evidence suitable for evidence-to-decision procedures. Compliance with this methodology is essential to implement AD biomarkers efficiently in clinical research and diagnostics. [ABSTRACT FROM AUTHOR]

Published

2021

35. Plasma Phospho‐Tau Identifies Alzheimer's Co‐Pathology in Patients with Lewy Body Disease.

Author

Hall, Sara, Janelidze, Shorena, Londos, Elisabet, Leuzy, Antoine, Stomrud, Erik, Dage, Jeffrey L., and Hansson, Oskar

Abstract

Background: Alzheimer's disease co‐pathology is common in dementia with Lewy bodies and Parkinson's disease with dementia (Lewy body disease) and can reliably be detected with positron emission tomography (PET) or cerebrospinal fluid (CSF) biomarkers. Recently developed blood biomarkers are more accessible and less expensive alternatives. Objective: To investigate if plasma phospho‐tau217 and phospho‐tau181 can detect Alzheimer's pathology in Lewy body disease with dementia. Methods: In this cross‐sectional study we investigated plasma phospho‐tau217 and phospho‐tau181 in 35 patients with Lewy body disease with dementia. Patients underwent tau‐PET imaging (18F‐RO948). Results: Plasma phospho‐tau217 correlated with plasma phospho‐tau181, CSF phospho‐tau217 (rs = 0.68, P < 0.001), and negatively with CSF β‐amyloid42/40 (rs = −0.52, P = 0.001). Plasma phospho‐tau217 and phospho‐tau181 correlated with tau‐PET signal in the temporal cortex (rs > 0.56, P < 0.001) and predicted abnormal tau‐PET status and β‐amyloid status (area under the curve > 0.78 and > 0.81, respectively). Conclusion: Plasma phospho‐tau might be a useful marker for Alzheimer's co‐pathology in Lewy body disease with dementia. © 2020 The Authors. Movement Disorders published by Wiley Periodicals LLC on behalf of International Parkinson and Movement Disorder Society. [ABSTRACT FROM AUTHOR]

Published

2021

36. The accumulation rate of tau aggregates is higher in females and younger amyloid-positive subjects.

Author

Smith, Ruben, Strandberg, Olof, Mattsson-Carlgren, Niklas, Leuzy, Antoine, Palmqvist, Sebastian, Pontecorvo, Michael J, Devous, Michael D, Ossenkoppele, Rik, and Hansson, Oskar

Subjects

*MILD cognitive impairment, *JUVENILE idiopathic arthritis, *ALZHEIMER'S disease, *EXPERIMENTAL design, *CHRONIC traumatic encephalopathy, *DIAGNOSIS, *HUMAN reproduction, *NERVE tissue proteins, *MAGNETIC resonance imaging, *GENOTYPES, *APOLIPOPROTEINS, *DEMENTIA, *PEPTIDES, *CEREBRAL cortex, *LONGITUDINAL method

Abstract

The development of tau-PET allows paired helical filament tau pathology to be visualized in vivo. Increased knowledge about conditions affecting the rate of tau accumulation could guide the development of therapies halting the progression of Alzheimer's disease. However, the factors modifying the rate of tau accumulation over time in Alzheimer's disease are still largely unknown. Large-scale longitudinal cohort studies, adjusting for baseline tau load, are needed to establish such risk factors. In the present longitudinal study, 419 participants from four cohorts in the USA (Avid 05e, n = 157; Expedition-3, n = 82; ADNI, n = 123) and Sweden (BioFINDER, n = 57) were scanned repeatedly with tau-PET. The study participants were cognitively unimpaired (n = 153), or patients with mild cognitive impairment (n = 139) or Alzheimer's disease dementia (n = 127). Participants underwent two to four tau-PET (18F-flortaucipir) scans with a mean (± standard deviation) of 537 (±163) days between the first and last scan. The change in tau-PET signal was estimated in temporal meta- and neocortical regions of interest. Subject specific tau-PET slopes were predicted simultaneously by age, sex, amyloid status (determined by amyloid-β PET), APOE ε4 genotype, study cohort, diagnosis and baseline tau load. We found that accelerated increase in tau-PET signal was observed in amyloid-β-positive mild cognitive impairment (3.0 ± 5.3%) and Alzheimer's disease dementia (2.9 ± 5.7%), respectively, when compared to either amyloid-β-negative cognitively unimpaired (0.4 ± 2.7%), amyloid-β-negative mild cognitive impairment (-0.4 ± 2.3%) or amyloid-β-positive cognitively unimpaired (1.2 ± 2.8%). Tau-PET uptake was accelerated in females (temporal region of interest: t = 2.86, P = 0.005; neocortical region of interest: t = 2.90, P = 0.004), younger individuals (temporal region of interest: t = -2.49, P = 0.013), and individuals with higher baseline tau-PET signal (temporal region of interest: t = 3.83, P < 0.001; neocortical region of interest: t = 5.01, P < 0.001). Tau-PET slopes decreased with age in amyloid-β-positive subjects, but were stable by age in amyloid-β-negative subjects (age × amyloid-β status interaction: t = -2.39, P = 0.018). There were no effects of study cohort or APOE ε4 positivity. In a similar analysis on longitudinal amyloid-β-PET (in ADNI subjects only, n = 639), we found significant associations between the rate of amyloid-β accumulation and APOE ε4 positivity, older age and baseline amyloid-β positivity, but no effect of sex. In conclusion, in this longitudinal PET study comprising four cohorts, we found that the tau accumulation rate is greater in females and younger amyloid-β-positive individuals, while amyloid-β accumulation is greater in APOE ε4 carriers and older individuals. These findings are important considerations for the design of clinical trials, and might improve our understanding of factors associated with faster tau aggregation and spread. [ABSTRACT FROM AUTHOR]

Published

2020

37. Blood and cerebrospinal fluid neurofilament light differentially detect neurodegeneration in early Alzheimer's disease.

Author

Andersson, Emelie, Janelidze, Shorena, Lampinen, Björn, Nilsson, Markus, Leuzy, Antoine, Stomrud, Erik, Blennow, Kaj, Zetterberg, Henrik, and Hansson, Oskar

Subjects

*CEREBROSPINAL fluid, *ALZHEIMER'S disease, *WHITE matter (Nerve tissue), *CYTOPLASMIC filaments, *MILD cognitive impairment

Abstract

Cerebrospinal fluid (CSF) neurofilament light (NfL) concentration has reproducibly been shown to reflect neurodegeneration in brain disorders, including Alzheimer's disease (AD). NfL concentration in blood correlates with the corresponding CSF levels, but few studies have directly compared the reliability of these 2 markers in sporadic AD. Herein, we measured plasma and CSF concentrations of NfL in 478 cognitively unimpaired (CU) subjects, 227 patients with mild cognitive impairment, and 113 patients with AD dementia. We found that the concentration of NfL in CSF, but not in plasma, was increased in response to Aβ pathology in CU subjects. Both CSF and plasma NfL concentrations were increased in patients with mild cognitive impairment and AD dementia. Furthermore, only NfL in CSF was associated with reduced white matter microstructure in CU subjects. Finally, in a transgenic mouse model of AD, CSF NfL increased before serum NfL in response to the development of Aβ pathology. In conclusion, NfL in CSF may be a more reliable biomarker of neurodegeneration than NfL in blood in preclinical sporadic AD. • CSF NfL is increased and associated with amyloid pathology in preclinical AD. • Plasma NfL is increased in symptomatic AD. • CSF NfL is associated with reduced white matter microstructure in preclinical AD. • Plasma NfL is associated with reduced white matter microstructure in symptomatic AD. • In 5xFAD mice, NfL in CSF is increased at an earlier time point than in serum. [ABSTRACT FROM AUTHOR]

Published

2020

38. Discriminative Accuracy of Plasma Phospho-tau217 for Alzheimer Disease vs Other Neurodegenerative Disorders.

Author

Palmqvist, Sebastian, Janelidze, Shorena, Quiroz, Yakeel T., Zetterberg, Henrik, Lopera, Francisco, Stomrud, Erik, Su, Yi, Chen, Yinghua, Serrano, Geidy E., Leuzy, Antoine, Mattsson-Carlgren, Niklas, Strandberg, Olof, Smith, Ruben, Villegas, Andres, Sepulveda-Falla, Diego, Chai, Xiyun, Proctor, Nicholas K., Beach, Thomas G., Blennow, Kaj, and Dage, Jeffrey L.

Subjects

*THREONINE, *BIOMARKERS, *ALZHEIMER'S disease, *NEURODEGENERATION, *DIAGNOSIS, *ALZHEIMER'S disease diagnosis, *RESEARCH, *NERVE tissue proteins, *GENETIC mutation, *CROSS-sectional method, *RESEARCH methodology, *PHARMACOKINETICS, *MAGNETIC resonance imaging, *EVALUATION research, *MEDICAL cooperation, *COMPARATIVE studies, *RESEARCH funding, *MEMBRANE proteins, *PEPTIDES

Abstract

Importance: There are limitations in current diagnostic testing approaches for Alzheimer disease (AD).Objective: To examine plasma tau phosphorylated at threonine 217 (P-tau217) as a diagnostic biomarker for AD.Design, Setting, and Participants: Three cross-sectional cohorts: an Arizona-based neuropathology cohort (cohort 1), including 34 participants with AD and 47 without AD (dates of enrollment, May 2007-January 2019); the Swedish BioFINDER-2 cohort (cohort 2), including cognitively unimpaired participants (n = 301) and clinically diagnosed patients with mild cognitive impairment (MCI) (n = 178), AD dementia (n = 121), and other neurodegenerative diseases (n = 99) (April 2017-September 2019); and a Colombian autosomal-dominant AD kindred (cohort 3), including 365 PSEN1 E280A mutation carriers and 257 mutation noncarriers (December 2013-February 2017).Exposures: Plasma P-tau217.Main Outcomes and Measures: Primary outcome was the discriminative accuracy of plasma P-tau217 for AD (clinical or neuropathological diagnosis). Secondary outcome was the association with tau pathology (determined using neuropathology or positron emission tomography [PET]).Results: Mean age was 83.5 (SD, 8.5) years in cohort 1, 69.1 (SD, 10.3) years in cohort 2, and 35.8 (SD, 10.7) years in cohort 3; 38% were women in cohort 1, 51% in cohort 2, and 57% in cohort 3. In cohort 1, antemortem plasma P-tau217 differentiated neuropathologically defined AD from non-AD (area under the curve [AUC], 0.89 [95% CI, 0.81-0.97]) with significantly higher accuracy than plasma P-tau181 and neurofilament light chain (NfL) (AUC range, 0.50-0.72; P < .05). The discriminative accuracy of plasma P-tau217 in cohort 2 for clinical AD dementia vs other neurodegenerative diseases (AUC, 0.96 [95% CI, 0.93-0.98]) was significantly higher than plasma P-tau181, plasma NfL, and MRI measures (AUC range, 0.50-0.81; P < .001) but not significantly different compared with cerebrospinal fluid (CSF) P-tau217, CSF P-tau181, and tau-PET (AUC range, 0.90-0.99; P > .15). In cohort 3, plasma P-tau217 levels were significantly greater among PSEN1 mutation carriers, compared with noncarriers, from approximately 25 years and older, which is 20 years prior to estimated onset of MCI among mutation carriers. Plasma P-tau217 levels correlated with tau tangles in participants with (Spearman ρ = 0.64; P < .001), but not without (Spearman ρ = 0.15; P = .33), β-amyloid plaques in cohort 1. In cohort 2, plasma P-tau217 discriminated abnormal vs normal tau-PET scans (AUC, 0.93 [95% CI, 0.91-0.96]) with significantly higher accuracy than plasma P-tau181, plasma NfL, CSF P-tau181, CSF Aβ42:Aβ40 ratio, and MRI measures (AUC range, 0.67-0.90; P < .05), but its performance was not significantly different compared with CSF P-tau217 (AUC, 0.96; P = .22).Conclusions and Relevance: Among 1402 participants from 3 selected cohorts, plasma P-tau217 discriminated AD from other neurodegenerative diseases, with significantly higher accuracy than established plasma- and MRI-based biomarkers, and its performance was not significantly different from key CSF- or PET-based measures. Further research is needed to optimize the assay, validate the findings in unselected and diverse populations, and determine its potential role in clinical care. [ABSTRACT FROM AUTHOR]

Published

2020

39. An update on blood-based biomarkers for non-Alzheimer neurodegenerative disorders.

Author

Ashton, Nicholas J., Hye, Abdul, Rajkumar, Anto P., Leuzy, Antoine, Snowden, Stuart, Suárez-Calvet, Marc, Karikari, Thomas K., Schöll, Michael, La Joie, Renaud, Rabinovici, Gil D., Höglund, Kina, Ballard, Clive, Hortobágyi, Tibor, Svenningsson, Per, Blennow, Kaj, Zetterberg, Henrik, and Aarsland, Dag

Subjects

*FRONTOTEMPORAL lobar degeneration, *NEURODEGENERATION, *LEWY body dementia, *CEREBROSPINAL fluid examination, *PARKINSONIAN disorders, *BIOMARKERS

Abstract

Cerebrospinal fluid analyses and neuroimaging can identify the underlying pathophysiology at the earliest stage of some neurodegenerative disorders, but do not have the scalability needed for population screening. Therefore, a blood-based marker for such pathophysiology would have greater utility in a primary care setting and in eligibility screening for clinical trials. Rapid advances in ultra-sensitive assays have enabled the levels of pathological proteins to be measured in blood samples, but research has been predominantly focused on Alzheimer disease (AD). Nonetheless, proteins that were identified as potential blood-based biomarkers for AD, for example, amyloid-β, tau, phosphorylated tau and neurofilament light chain, are likely to be relevant to other neurodegenerative disorders that involve similar pathological processes and could also be useful for the differential diagnosis of clinical symptoms. This Review outlines the neuropathological, clinical, molecular imaging and cerebrospinal fluid features of the most common neurodegenerative disorders outside the AD continuum and gives an overview of the current status of blood-based biomarkers for these disorders. [ABSTRACT FROM AUTHOR]

Published

2020

40. Quantitative positron emission tomography in brain research.

Author

Heurling, Kerstin, Jonasson, My, Lubberink, Mark, Leuzy, Antoine, Nordberg, Agneta, Frick, Andreas, and Zimmer, Eduardo R.

Subjects

*POSITRON emission tomography, *ALZHEIMER'S disease, *PARKINSON'S disease, *BRAIN imaging, DIAGNOSIS of brain abnormalities

Abstract

The application of positron emission tomography (PET) in brain research has increased substantially during the past 20 years, and is still growing. PET provides a unique insight into physiological and pathological processes in vivo. In this article we introduce the fundamentals of PET, and the methods available for acquiring quantitative estimates of the parameters of interest. A short introduction to different areas of application is also given, including basic research of brain function and in neurology, psychiatry, drug receptor occupancy studies, and its application in diagnostics of neurodegenerative disorders such as Alzheimer’s disease and Parkinson’s disease. Our aim is to inform the unfamiliar reader of the underlying basics and potential applications of PET, hoping to inspire the reader into considering how the technique could be of benefit for his or her own research. [ABSTRACT FROM AUTHOR]

Published

2017

41. Tau PET imaging: present and future directions.

Author

Saint-Aubert, Laure, Lemoine, Laetitia, Chiotis, Konstantinos, Leuzy, Antoine, Rodriguez-Vieitez, Elena, and Nordberg, Agneta

Subjects

*POSITRON emission tomography, *NEURODEGENERATION, *TREATMENT of neurodegeneration, *ALZHEIMER'S disease treatment, *BRAIN imaging, *DIAGNOSIS

Abstract

Abnormal aggregation of tau in the brain is a major contributing factor in various neurodegenerative diseases. The role of tau phosphorylation in the pathophysiology of tauopathies remains unclear. Consequently, it is important to be able to accurately and specifically target tau deposits in vivo in the brains of patients. The advances of molecular imaging in the recent years have now led to the recent development of promising tau-specific tracers for positron emission tomography (PET), such as THK5317, THK5351, AV-1451, and PBB3. These tracers are now available for clinical assessment in patients with various tauopathies, including Alzheimer's disease, as well as in healthy subjects. Exploring the patterns of tau deposition in vivo for different pathologies will allow discrimination between neurodegenerative diseases, including different tauopathies, and monitoring of disease progression. The variety and complexity of the different types of tau deposits in the different diseases, however, has resulted in quite a challenge for the development of tau PET tracers. Extensive work remains in order to fully characterize the binding properties of the tau PET tracers, and to assess their usefulness as an early biomarker of the underlying pathology. In this review, we summarize recent findings on the most promising tau PET tracers to date, discuss what has been learnt from these findings, and offer some suggestions for the next steps that need to be achieved in a near future. [ABSTRACT FROM AUTHOR]

Published

2017

42. Tau pet imaging in neurodegenerative tauopathies – a multimodal paradigm.

Author

Chiotis, Konstantinos, Saint-Aubert, Laure, Leuzy, Antoine, Rodriguez-Vieitez, Elena, and Nordberg, Agneta

Subjects

*NEURODEGENERATION, *TAU proteins, *POSITRON emission tomography, *NEUROBIOLOGY, *AGE factors in disease

Published

2016

43. Dissociation between Brain Amyloid Deposition and Metabolism in Early Mild Cognitive Impairment.

Author

Liyong Wu, Rowley, Jared, Mohades, Sara, Leuzy, Antoine, Dauar, Marina Tedeschi, Shin, Monica, Fonov, Vladimir, Jianping Jia, Gauthier, Serge, and Rosa-Neto, Pedro

Subjects

*ALZHEIMER'S disease research, *COGNITION disorders research, *AMYLOID, *AMYLOIDOSIS, *BIOMARKERS, *METABOLISM

Abstract

Background: The hypothetical model of dynamic biomarkers for Alzheimer's disease (AD) describes high amyloid eposition and hypometabolism at the mild cognitive impairment (MCI) stage. However, it remains unknown whether brain myloidosis and hypometabolism follow the same trajectories in MCI individuals. We used the concept of early MCI (EMCI) nd late MCI (LMCI) as defined by the Alzheimer's disease Neuroimaging Initiative (ADNI)-Go in order to compare the iomarker profile between EMCI and LMCI. Objectives: To examine the global and voxel-based neocortical amyloid burden and metabolism among individuals who are ognitively normal (CN), as well as those with EMCI, LMCI and mild AD. Methods: In the present study, 354 participants, including CN (n = 109), EMCI (n = 157), LMCI (n = 39) and AD (n = 49), were nrolled between September 2009 and November 2011 through ADNI-GO and ADNI-2. Brain amyloid load and metabolism were estimated using [18F]AV45 and [18F]fluorodeoxyglucose ([18F]FDG) PET, respectively. Uptake ratio images of [18F]AV45 nd [18F]FDG were calculated by dividing the summed PET image by the median counts of the grey matter of the erebellum and pons, respectively. Group differences of global [18F]AV45 and [18F]FDG were analyzed using ANOVA, while he voxel-based group differences were estimated using statistic parametric mapping (SPM). Results: EMCI patients showed higher global [18F]AV45 retention compared to CN and lower uptake compared to LMCI. PM detected higher [18F]AV45 uptake in EMCI compared to CN in the precuneus, posterior cingulate, medial and dorsal ateral prefrontal cortices, bilaterally. EMCI showed lower [18F]AV45 retention than LMCI in the superior temporal, inferior arietal, as well as dorsal lateral prefrontal cortices, bilaterally. Regarding to the global [18F]FDG, EMCI patients showed no ignificant difference from CN and a higher uptake ratio compared to LMCI. At the voxel level, EMCI showed higher metabolism in precuneus, hippocampus, entorhinal and inferior parietal cortices, as compared to LMCI. Conclusions: The present results indicate that brain metabolism remains normal despite the presence of significant amyloid ccumulation in EMCI. These results suggest a role for anti-amyloid interventions in EMCI aiming to delay or halt the eposition of amyloid and related metabolism impairment. [ABSTRACT FROM AUTHOR]

Published

2012

44. Epistasis analysis links immune cascades and cerebral amyloidosis.

Author

Benedet, Andréa L, Labbe, Aurélie, Lemay, Philippe, Zimmer, Eduardo R, Pascoal, Tharick A, Leuzy, Antoine, Mathotaarachchi, Sulantha, Mohades, Sara, Shin, Monica, Dionne-Laporte, Alexandre, Beaudry, Thomas, Picard, Cynthia, Gauthier, Serge, Poirier, Judes, Rouleau, Guy, Rosa-Neto, Pedro, and Alzheimer’s Disease Neuroimaging Initiative

Subjects

*ALZHEIMER'S disease diagnosis, *AMYLOIDOSIS diagnosis, *COGNITION disorders diagnosis, *ALZHEIMER'S disease, *AMYLOIDOSIS, *COGNITION disorders, *GENES, *RESEARCH funding

Abstract

Background: Several lines of evidence suggest the involvement of neuroinflammatory changes in Alzheimer's disease (AD) pathophysiology such as amyloidosis and neurodegeneration. In fact, genome-wide association studies (GWAS) have shown a link between genes involved in neuroinflammation and AD. In order to further investigate whether interactions between candidate genetic variances coding for neuroinflammatory molecules are associated with brain amyloid β (Aβ) fibrillary accumulation, we conducted an epistasis analysis on a pool of genes associated with molecular mediators of inflammation.Methods: [(18)F]Florbetapir positron emission tomography (PET) imaging was employed to assess brain Aβ levels in 417 participants from ADNI-GO/2 and posteriorly 174 from ADNI-1. IL-1β, IL4, IL6, IL6r, IL10, IL12, IL18, C5, and C9 genes were chosen based on previous studies conducted in AD patients. Using the [(18)F]florbetapir standardized uptake value ratio (SUVR) as a quantitative measure of fibrillary Aβ, epistasis analyses were performed between two sets of markers of immune-related genes using gender, diagnosis, and apolipoprotein E (APOE) as covariates. Voxel-based analyses were also conducted. The results were corrected for multiple comparison tests. Cerebrospinal fluid (CSF) Aβ1-42/phosphorylated tau (p-tau) ratio concentrations were used to confirm such associations.Results: Epistasis analysis unveiled two significant single nucleotide polymorphism (SNP)-SNP interactions (false discovery rate (FDR) threshold 0.1), both interactions between C9 gene (rs261752) and IL6r gene (rs4240872, rs7514452). In a combined sample, the interactions were confirmed (p ≤ 10-5) and associated with amyloid accumulation within cognitively normal and AD spectrum groups. Voxel-based analysis corroborated initial findings. CSF biomarker (Aβ1-42/p-tau) confirmed the genetic interaction. Additionally, rs4240872 and rs7514452 SNPs were shown to be associated with CSF and plasma concentrations of IL6r protein.Conclusions: Certain allele combinations involving IL6r and C9 genes are associated with Aβ burden in the brain. Hypothesis-driven search for epistasis is a valuable strategy for investigating imaging endophenotypes in complex neurodegenerative diseases. [ABSTRACT FROM AUTHOR]

Published

2015