Your search keyword '"Holtzman, DM"' showing total 8 results

1. Spatial patterns of neuroimaging biomarker change in individuals from families with autosomal dominant Alzheimer's disease: a longitudinal study

Author

Gordon, BA, Blazey, TM, Su, Y, Hari-Raj, A, Dincer, A, Flores, S, Christensen, J, McDade, E, Wang, G, Xiong, C, Cairns, NJ, Hassenstab, J, Marcus, DS, Fagan, AM, Jack, CR, Hornbeck, RC, Paumier, KL, Ances, BM, Berman, SB, Brickman, AM, Cash, DM, Chhatwal, JP, Correia, S, Förster, S, Fox, NC, Graff-Radford, NR, la Fougère, C, Levin, J, Masters, CL, Rossor, MN, Salloway, S, Saykin, AJ, Schofield, PR, Thompson, PM, Weiner, MM, Holtzman, DM, Raichle, ME, Morris, JC, Bateman, RJ, Benzinger, TLS, Gordon, BA, Blazey, TM, Su, Y, Hari-Raj, A, Dincer, A, Flores, S, Christensen, J, McDade, E, Wang, G, Xiong, C, Cairns, NJ, Hassenstab, J, Marcus, DS, Fagan, AM, Jack, CR, Hornbeck, RC, Paumier, KL, Ances, BM, Berman, SB, Brickman, AM, Cash, DM, Chhatwal, JP, Correia, S, Förster, S, Fox, NC, Graff-Radford, NR, la Fougère, C, Levin, J, Masters, CL, Rossor, MN, Salloway, S, Saykin, AJ, Schofield, PR, Thompson, PM, Weiner, MM, Holtzman, DM, Raichle, ME, Morris, JC, Bateman, RJ, and Benzinger, TLS

Abstract

Background: Models of Alzheimer's disease propose a sequence of amyloid β (Aβ) accumulation, hypometabolism, and structural decline that precedes the onset of clinical dementia. These pathological features evolve both temporally and spatially in the brain. In this study, we aimed to characterise where in the brain and when in the course of the disease neuroimaging biomarkers become abnormal. Methods: Between Jan 1, 2009, and Dec 31, 2015, we analysed data from mutation non-carriers, asymptomatic carriers, and symptomatic carriers from families carrying gene mutations in presenilin 1 (PSEN1), presenilin 2 (PSEN2), or amyloid precursor protein (APP) enrolled in the Dominantly Inherited Alzheimer's Network. We analysed 11C-Pittsburgh Compound B (11C-PiB) PET, 18F-Fluorodeoxyglucose (18F-FDG) PET, and structural MRI data using regions of interest to assess change throughout the brain. We estimated rates of biomarker change as a function of estimated years to symptom onset at baseline using linear mixed-effects models and determined the earliest point at which biomarker trajectories differed between mutation carriers and non-carriers. This study is registered at ClinicalTrials.gov (number NCT00869817) Findings: 11C-PiB PET was available for 346 individuals (162 with longitudinal imaging), 18F-FDG PET was available for 352 individuals (175 with longitudinal imaging), and MRI data were available for 377 individuals (201 with longitudinal imaging). We found a sequence to pathological changes, with rates of Aβ deposition in mutation carriers being significantly different from those in non-carriers first (across regions that showed a significant difference, at a mean of 18·9 years [SD 3·3] before expected onset), followed by hypometabolism (14·1 years [5·1] before expected onset), and lastly structural decline (4·7 years [4·2] before expected onset). This biomarker ordering was preserved in most, but not all, regions. The temporal emergence within a biomarker varied across th

Published

2018

2. White matter hyperintensities and the mediating role of cerebral amyloid angiopathy in dominantly-inherited Alzheimer’s disease

Author

Lee, S, Zimmerman, ME, Narkhede, A, Nasrabady, SE, Tosto, G, Meier, IB, Benzinger, TLS, Marcus, DS, Fagan, AM, Fox, NC, Cairns, NJ, Holtzman, DM, Buckles, V, Ghetti, B, McDade, E, Martins, RN, Saykin, AJ, Masters, CL, Ringman, JM, Fӧrster, S, Schofield, PR, Sperling, RA, Johnson, KA, Chhatwal, JP, Salloway, S, Correia, S, Jack, CR, Weiner, M, Bateman, RJ, Morris, JC, Mayeux, R, Brickman, AM, Lee, S, Zimmerman, ME, Narkhede, A, Nasrabady, SE, Tosto, G, Meier, IB, Benzinger, TLS, Marcus, DS, Fagan, AM, Fox, NC, Cairns, NJ, Holtzman, DM, Buckles, V, Ghetti, B, McDade, E, Martins, RN, Saykin, AJ, Masters, CL, Ringman, JM, Fӧrster, S, Schofield, PR, Sperling, RA, Johnson, KA, Chhatwal, JP, Salloway, S, Correia, S, Jack, CR, Weiner, M, Bateman, RJ, Morris, JC, Mayeux, R, and Brickman, AM

Abstract

Introduction White matter hyperintensity (WMH) volume on MRI is increased among presymptomatic individuals with autosomal dominant mutations for Alzheimer’s disease (AD). One potential explanation is that WMH, conventionally considered a marker of cerebrovascular disease, are a reflection of cerebral amyloid angiopathy (CAA) and that increased WMH in this population is a manifestation of this vascular form of primary AD pathology. We examined whether the presence of cerebral microbleeds, a marker of CAA, mediates the relationship between WMH and estimated symptom onset in individuals with and without autosomal dominant mutations for AD. Participants and methods Participants (n = 175, mean age = 41.1 years) included 112 with an AD mutation and 63 first-degree non-carrier controls. We calculated the estimated years from expected symptom onset (EYO) and analyzed baseline MRI data for WMH volume and presence of cerebral microbleeds. Mixed effects regression and tests of mediation were used to examine microbleed and WMH differences between carriers and non-carriers and to test the whether the association between WMH and mutation status is dependent on the presence of microbleeds. Results Mutation carriers were more likely to have microbleeds than non-carriers (p<0.05) and individuals with microbleeds had higher WMH volume than those without (p<0.05). Total WMH volume was increased in mutation carriers compared with non-carriers, up to 20 years prior to EYO, after controlling for microbleed status, as we demonstrated previously. Formal testing of mediation demonstrated that 21% of the association between mutation status and WMH was mediated by presence of microbleeds (p = 0.03) but a significant direct effect of WMH remained (p = 0.02) after controlling for presence of microbleeds. Discussion Although there is some co-dependency between WMH and microbleeds, the observed increases in WMH among mutation carriers does not appear to be fully mediated by this marker of CAA. Th

Published

2018

3. White matter hyperintensities and the mediating role of cerebral amyloid angiopathy in dominantly-inherited Alzheimer's disease

Author

Ginsberg, SD, Lee, S, Zimmerman, ME, Narkhede, A, Nasrabady, SE, Tosto, G, Meier, IB, Benzinger, TLS, Marcus, DS, Fagan, AM, Fox, NC, Cairns, NJ, Holtzman, DM, Buckles, V, Ghetti, B, McDade, E, Martins, RN, Saykin, AJ, Masters, CL, Ringman, JM, Foerster, S, Schofield, PR, Sperling, RA, Johnson, KA, Chhatwal, JP, Salloway, S, Correia, S, Jack, CR, Weiner, M, Bateman, RJ, Morris, JC, Mayeux, R, Brickman, AM, Ginsberg, SD, Lee, S, Zimmerman, ME, Narkhede, A, Nasrabady, SE, Tosto, G, Meier, IB, Benzinger, TLS, Marcus, DS, Fagan, AM, Fox, NC, Cairns, NJ, Holtzman, DM, Buckles, V, Ghetti, B, McDade, E, Martins, RN, Saykin, AJ, Masters, CL, Ringman, JM, Foerster, S, Schofield, PR, Sperling, RA, Johnson, KA, Chhatwal, JP, Salloway, S, Correia, S, Jack, CR, Weiner, M, Bateman, RJ, Morris, JC, Mayeux, R, and Brickman, AM

Abstract

INTRODUCTION: White matter hyperintensity (WMH) volume on MRI is increased among presymptomatic individuals with autosomal dominant mutations for Alzheimer's disease (AD). One potential explanation is that WMH, conventionally considered a marker of cerebrovascular disease, are a reflection of cerebral amyloid angiopathy (CAA) and that increased WMH in this population is a manifestation of this vascular form of primary AD pathology. We examined whether the presence of cerebral microbleeds, a marker of CAA, mediates the relationship between WMH and estimated symptom onset in individuals with and without autosomal dominant mutations for AD. PARTICIPANTS AND METHODS: Participants (n = 175, mean age = 41.1 years) included 112 with an AD mutation and 63 first-degree non-carrier controls. We calculated the estimated years from expected symptom onset (EYO) and analyzed baseline MRI data for WMH volume and presence of cerebral microbleeds. Mixed effects regression and tests of mediation were used to examine microbleed and WMH differences between carriers and non-carriers and to test the whether the association between WMH and mutation status is dependent on the presence of microbleeds. RESULTS: Mutation carriers were more likely to have microbleeds than non-carriers (p<0.05) and individuals with microbleeds had higher WMH volume than those without (p<0.05). Total WMH volume was increased in mutation carriers compared with non-carriers, up to 20 years prior to EYO, after controlling for microbleed status, as we demonstrated previously. Formal testing of mediation demonstrated that 21% of the association between mutation status and WMH was mediated by presence of microbleeds (p = 0.03) but a significant direct effect of WMH remained (p = 0.02) after controlling for presence of microbleeds. DISCUSSION: Although there is some co-dependency between WMH and microbleeds, the observed increases in WMH among mutation carriers does not appear to be fully mediated by this marker of CAA

Published

2018

4. White matter hyperintensities are a core feature of Alzheimer's disease: Evidence from the dominantly inherited Alzheimer network

Author

Lee, S, Viqar, F, Zimmerman, ME, Narkhede, A, Tosto, G, Benzinger, TLS, Marcus, DS, Fagan, AM, Goate, A, Fox, NC, Cairns, NJ, Holtzman, DM, Buckles, V, Ghetti, B, McDade, E, Martins, RN, Saykin, AJ, Masters, CL, Ringman, JM, Ryan, NS, Förster, S, Laske, C, Schofield, PR, Sperling, RA, Salloway, S, Correia, S, Jack, C, Weiner, M, Bateman, RJ, Morris, JC, Mayeux, R, Brickman, AM, Lee, S, Viqar, F, Zimmerman, ME, Narkhede, A, Tosto, G, Benzinger, TLS, Marcus, DS, Fagan, AM, Goate, A, Fox, NC, Cairns, NJ, Holtzman, DM, Buckles, V, Ghetti, B, McDade, E, Martins, RN, Saykin, AJ, Masters, CL, Ringman, JM, Ryan, NS, Förster, S, Laske, C, Schofield, PR, Sperling, RA, Salloway, S, Correia, S, Jack, C, Weiner, M, Bateman, RJ, Morris, JC, Mayeux, R, and Brickman, AM

Abstract

Objective White matter hyperintensities (WMHs) are areas of increased signal on T2-weighted magnetic resonance imaging (MRI) scans that most commonly reflect small vessel cerebrovascular disease. Increased WMH volume is associated with risk and progression of Alzheimer's disease (AD). These observations are typically interpreted as evidence that vascular abnormalities play an additive, independent role contributing to symptom presentation, but not core features of AD. We examined the severity and distribution of WMH in presymptomatic PSEN1, PSEN2, and APP mutation carriers to determine the extent to which WMH manifest in individuals genetically determined to develop AD. Methods The study comprised participants (n = 299; age = 39.03 ± 10.13) from the Dominantly Inherited Alzheimer Network, including 184 (61.5%) with a mutation that results in AD and 115 (38.5%) first-degree relatives who were noncarrier controls. We calculated the estimated years from expected symptom onset (EYO) by subtracting the affected parent's symptom onset age from the participant's age. Baseline MRI data were analyzed for total and regional WMH. Mixed-effects piece-wise linear regression was used to examine WMH differences between carriers and noncarriers with respect to EYO. Results Mutation carriers had greater total WMH volumes, which appeared to increase approximately 6 years before expected symptom onset. Effects were most prominent for the parietal and occipital lobe, which showed divergent effects as early as 22 years before estimated onset. Interpretation Autosomal-dominant AD is associated with increased WMH well before expected symptom onset. The findings suggest the possibility that WMHs are a core feature of AD, a potential therapeutic target, and a factor that should be integrated into pathogenic models of the disease.

Published

2016

5. White Matter Hyperintensities Are a Core Feature of Alzheimer's Disease: Evidence from the Dominantly Inherited Alzheimer Network

Author

Lee, S, Viqar, F, Zimmerman, ME, Narkhede, A, Tosto, G, Benzinger, TLS, Marcus, DS, Fagan, AM, Goate, A, Fox, NC, Cairns, NJ, Holtzman, DM, Buckles, V, Ghetti, B, McDade, E, Martins, RN, Saykin, AJ, Masters, CL, Ringman, JM, Ryan, NS, Forster, S, Laske, C, Schofield, PR, Sperling, RA, Salloway, S, Correia, S, Jack, C, Weiner, M, Bateman, RJ, Morris, JC, Mayeux, R, Brickman, AM, Lee, S, Viqar, F, Zimmerman, ME, Narkhede, A, Tosto, G, Benzinger, TLS, Marcus, DS, Fagan, AM, Goate, A, Fox, NC, Cairns, NJ, Holtzman, DM, Buckles, V, Ghetti, B, McDade, E, Martins, RN, Saykin, AJ, Masters, CL, Ringman, JM, Ryan, NS, Forster, S, Laske, C, Schofield, PR, Sperling, RA, Salloway, S, Correia, S, Jack, C, Weiner, M, Bateman, RJ, Morris, JC, Mayeux, R, and Brickman, AM

Abstract

OBJECTIVE: White matter hyperintensities (WMHs) are areas of increased signal on T2-weighted magnetic resonance imaging (MRI) scans that most commonly reflect small vessel cerebrovascular disease. Increased WMH volume is associated with risk and progression of Alzheimer's disease (AD). These observations are typically interpreted as evidence that vascular abnormalities play an additive, independent role contributing to symptom presentation, but not core features of AD. We examined the severity and distribution of WMH in presymptomatic PSEN1, PSEN2, and APP mutation carriers to determine the extent to which WMH manifest in individuals genetically determined to develop AD. METHODS: The study comprised participants (n = 299; age = 39.03 ± 10.13) from the Dominantly Inherited Alzheimer Network, including 184 (61.5%) with a mutation that results in AD and 115 (38.5%) first-degree relatives who were noncarrier controls. We calculated the estimated years from expected symptom onset (EYO) by subtracting the affected parent's symptom onset age from the participant's age. Baseline MRI data were analyzed for total and regional WMH. Mixed-effects piece-wise linear regression was used to examine WMH differences between carriers and noncarriers with respect to EYO. RESULTS: Mutation carriers had greater total WMH volumes, which appeared to increase approximately 6 years before expected symptom onset. Effects were most prominent for the parietal and occipital lobe, which showed divergent effects as early as 22 years before estimated onset. INTERPRETATION: Autosomal-dominant AD is associated with increased WMH well before expected symptom onset. The findings suggest the possibility that WMHs are a core feature of AD, a potential therapeutic target, and a factor that should be integrated into pathogenic models of the disease. Ann Neurol 2016;79:929-939.

Published

2016

6. Functional connectivity in autosomal dominant and late-onset Alzheimer disease

Author

Thomas, JB, Brier, MR, Bateman, RJ, Snyder, AZ, Benzinger, TL, Xiong, C, Raichle, M, Holtzman, DM, Sperling, RA, Mayeux, R, Ghetti, B, Ringman, JM, Salloway, S, McDade, E, Rossor, MN, Ourselin, S, Schofield, PR, Masters, CL, Martins, RN, Weiner, MW, Thompson, PM, Fox, NC, Koeppe, RA, Jack, CR, Mathis, CA, Oliver, A, Blazey, TM, Moulder, K, Buckles, V, Hornbeck, R, Chhatwal, J, Schultz, AP, Goate, AM, Fagan, AM, Cairns, NJ, Marcus, DS, Morris, JC, Ances, BM, Thomas, JB, Brier, MR, Bateman, RJ, Snyder, AZ, Benzinger, TL, Xiong, C, Raichle, M, Holtzman, DM, Sperling, RA, Mayeux, R, Ghetti, B, Ringman, JM, Salloway, S, McDade, E, Rossor, MN, Ourselin, S, Schofield, PR, Masters, CL, Martins, RN, Weiner, MW, Thompson, PM, Fox, NC, Koeppe, RA, Jack, CR, Mathis, CA, Oliver, A, Blazey, TM, Moulder, K, Buckles, V, Hornbeck, R, Chhatwal, J, Schultz, AP, Goate, AM, Fagan, AM, Cairns, NJ, Marcus, DS, Morris, JC, and Ances, BM

Abstract

IMPORTANCE: Autosomal dominant Alzheimer disease (ADAD) is caused by rare genetic mutations in 3 specific genes in contrast to late-onset Alzheimer disease (LOAD), which has a more polygenetic risk profile. OBJECTIVE: To assess the similarities and differences in functional connectivity changes owing to ADAD and LOAD. DESIGN, SETTING, AND PARTICIPANTS: We analyzed functional connectivity in multiple brain resting state networks (RSNs) in a cross-sectional cohort of participants with ADAD (n = 79) and LOAD (n = 444), using resting-state functional connectivitymagnetic resonance imaging at multiple international academic sites. MAIN OUTCOMES AND MEASURES: For both types of AD, we quantified and compared functional connectivity changes in RSNs as a function of dementia severity measured by the Clinical Dementia Rating Scale. In ADAD, we qualitatively investigated functional connectivity changes with respect to estimated years from onset of symptoms within 5 RSNs. RESULTS: A decrease in functional connectivity with increasing Clinical Dementia Rating scores were similar for both LOAD and ADAD in multiple RSNs. Ordinal logistic regression models constructed in one type of Alzheimer disease accurately predicted clinical dementia rating scores in the other, further demonstrating the similarity of functional connectivity loss in each disease type. Among participants with ADAD, functional connectivity in multiple RSNs appeared qualitatively lower in asymptomatic mutation carriers near their anticipated age of symptom onset compared with asymptomatic mutation noncarriers. CONCLUSIONS AND RELEVANCE: Resting-state functional connectivity magnetic resonance imaging changes with progressing AD severity are similar between ADAD and LOAD. Resting-state functional connectivitymagnetic resonance imagingmay be a useful end point for LOAD and ADAD therapy trials. Moreover, the disease process of ADAD may be an effective model for the LOAD disease process.

Published

2014

7. Functional Connectivity in Autosomal Dominant and Late-Onset Alzheimer Disease

Author

Thomas, JB, Brier, MR, Bateman, RJ, Snyder, AZ, Benzinger, TL, Xiong, C, Raichle, M, Holtzman, DM, Sperling, RA, Mayeux, R, Ghetti, B, Ringman, JM, Salloway, S, McDade, E, Rossor, MN, Ourselin, S, Schofield, PR, Masters, CL, Martins, RN, Weiner, MW, Thompson, PM, Fox, NC, Koeppe, RA, Jack, CR, Mathis, CA, Oliver, A, Blazey, TM, Moulder, K, Buckles, V, Hornbeck, R, Chhatwal, J, Schultz, AP, Goate, AM, Fagan, AM, Cairns, NJ, Marcus, DS, Morris, JC, Ances, BM, Thomas, JB, Brier, MR, Bateman, RJ, Snyder, AZ, Benzinger, TL, Xiong, C, Raichle, M, Holtzman, DM, Sperling, RA, Mayeux, R, Ghetti, B, Ringman, JM, Salloway, S, McDade, E, Rossor, MN, Ourselin, S, Schofield, PR, Masters, CL, Martins, RN, Weiner, MW, Thompson, PM, Fox, NC, Koeppe, RA, Jack, CR, Mathis, CA, Oliver, A, Blazey, TM, Moulder, K, Buckles, V, Hornbeck, R, Chhatwal, J, Schultz, AP, Goate, AM, Fagan, AM, Cairns, NJ, Marcus, DS, Morris, JC, and Ances, BM

Abstract

IMPORTANCE: Autosomal dominant Alzheimer disease (ADAD) is caused by rare genetic mutations in 3 specific genes in contrast to late-onset Alzheimer disease (LOAD), which has a more polygenetic risk profile. OBJECTIVE: To assess the similarities and differences in functional connectivity changes owing to ADAD and LOAD. DESIGN, SETTING, AND PARTICIPANTS: We analyzed functional connectivity in multiple brain resting state networks (RSNs) in a cross-sectional cohort of participants with ADAD (n = 79) and LOAD (n = 444), using resting-state functional connectivity magnetic resonance imaging at multiple international academic sites. MAIN OUTCOMES AND MEASURES: For both types of AD, we quantified and compared functional connectivity changes in RSNs as a function of dementia severity measured by the Clinical Dementia Rating Scale. In ADAD, we qualitatively investigated functional connectivity changes with respect to estimated years from onset of symptoms within 5 RSNs. RESULTS: A decrease in functional connectivity with increasing Clinical Dementia Rating scores were similar for both LOAD and ADAD in multiple RSNs. Ordinal logistic regression models constructed in one type of Alzheimer disease accurately predicted clinical dementia rating scores in the other, further demonstrating the similarity of functional connectivity loss in each disease type. Among participants with ADAD, functional connectivity in multiple RSNs appeared qualitatively lower in asymptomatic mutation carriers near their anticipated age of symptom onset compared with asymptomatic mutation noncarriers. CONCLUSIONS AND RELEVANCE: Resting-state functional connectivity magnetic resonance imaging changes with progressing AD severity are similar between ADAD and LOAD. Resting-state functional connectivity magnetic resonance imaging may be a useful end point for LOAD and ADAD therapy trials. Moreover, the disease process of ADAD may be an effective model for the LOAD disease process.

Published

2014

8. Regional variability of imaging biomarkers in autosomal dominant Alzheimer's disease

Author

Benzinger, TLS, Blazey, T, Jack, CR, Koeppe, RA, Su, Y, Xiong, C, Raichle, ME, Snyder, AZ, Ances, BM, Bateman, RJ, Cairns, NJ, Fagan, AM, Goate, A, Marcus, DS, Aisen, PS, Christensen, JJ, Ercole, L, Hornbeck, RC, Farrar, AM, Aldea, P, Jasielec, MS, Owen, CJ, Xie, X, Mayeux, R, Brickman, A, McDade, E, Klunk, W, Mathis, CA, Ringman, J, Thompson, PM, Ghetti, B, Saykin, AJ, Sperling, RA, Johnson, KA, Salloway, S, Correia, S, Schofield, PR, Masters, CL, Rowe, C, Villemagne, VL, Martins, R, Ourselin, S, Rossor, MN, Fox, NC, Cash, DM, Weiner, MW, Holtzman, DM, Buckles, VD, Moulder, K, Morris, JC, Benzinger, TLS, Blazey, T, Jack, CR, Koeppe, RA, Su, Y, Xiong, C, Raichle, ME, Snyder, AZ, Ances, BM, Bateman, RJ, Cairns, NJ, Fagan, AM, Goate, A, Marcus, DS, Aisen, PS, Christensen, JJ, Ercole, L, Hornbeck, RC, Farrar, AM, Aldea, P, Jasielec, MS, Owen, CJ, Xie, X, Mayeux, R, Brickman, A, McDade, E, Klunk, W, Mathis, CA, Ringman, J, Thompson, PM, Ghetti, B, Saykin, AJ, Sperling, RA, Johnson, KA, Salloway, S, Correia, S, Schofield, PR, Masters, CL, Rowe, C, Villemagne, VL, Martins, R, Ourselin, S, Rossor, MN, Fox, NC, Cash, DM, Weiner, MW, Holtzman, DM, Buckles, VD, Moulder, K, and Morris, JC

Abstract

Major imaging biomarkers of Alzheimer's disease include amyloid deposition [imaged with [(11)C]Pittsburgh compound B (PiB) PET], altered glucose metabolism (imaged with [(18)F]fluro-deoxyglucose PET), and structural atrophy (imaged by MRI). Recently we published the initial subset of imaging findings for specific regions in a cohort of individuals with autosomal dominant Alzheimer's disease. We now extend this work to include a larger cohort, whole-brain analyses integrating all three imaging modalities, and longitudinal data to examine regional differences in imaging biomarker dynamics. The anatomical distribution of imaging biomarkers is described in relation to estimated years from symptom onset. Autosomal dominant Alzheimer's disease mutation carrier individuals have elevated PiB levels in nearly every cortical region 15 y before the estimated age of onset. Reduced cortical glucose metabolism and cortical thinning in the medial and lateral parietal lobe appeared 10 and 5 y, respectively, before estimated age of onset. Importantly, however, a divergent pattern was observed subcortically. All subcortical gray-matter regions exhibited elevated PiB uptake, but despite this, only the hippocampus showed reduced glucose metabolism. Similarly, atrophy was not observed in the caudate and pallidum despite marked amyloid accumulation. Finally, before hypometabolism, a hypermetabolic phase was identified for some cortical regions, including the precuneus and posterior cingulate. Additional analyses of individuals in which longitudinal data were available suggested that an accelerated appearance of volumetric declines approximately coincides with the onset of the symptomatic phase of the disease.

Published

2013