Increased metabolic vulnerability in early-onset Alzheimer’s disease is not related to amyloid burden

Rabinovici, Gil D.; Furst, Ansgar J.; Alkalay, Adi; Racine, Caroline A.; O’Neil, James P.; Janabi, Mustafa; Baker, Suzanne L.; Agarwal, Neha; Bonasera, Stephen J.; Mormino, Elizabeth C.; Weiner, Michael W.; Gorno‐Tempini, Maria Luisa; Rosen, Howard J.; Miller, Bruce L.; Jagust, William J.

doi:10.1093/brain/awp326

Cited by 246 publications

(215 citation statements)

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“…25 Given the differential atrophy patterns seen in AD and PCA, 26 we corrected PET data for atrophy by applying a 2-compartmental partial volume correction 27 to all subjects with an MRI (10/12 PCA, 12/14 AD, and all NC) (see appendix e-1). 15,27 Since the benefit of partial volume correction for PiB data are controversial, all primary analyses were performed using uncorrected PET data, while confirmatory analyses were conducted with atrophy-corrected data in the subset of patients with an MRI.…”

Section: Methods Study Population Patients Were Recruitedmentioning

confidence: 99%

“…Based on the preponderance of postmortem data and previously demonstrated dissociations between PiB binding and clinical features of AD, 14,15 we hypothesized that patients with PCA would show diffuse cortical PiB binding in a pattern indistinguishable from clinically "typical" AD, but greater glucose hypometabolism than patients with AD in occipital cortex, correlating with their selective impairment in visual processing.…”

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confidence: 99%

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Distinct clinical and metabolic deficits in PCA and AD are not related to amyloid distribution

Rosenbloom¹,

Alkalay²,

Agarwal³

et al. 2011

Neurology

118

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Section: Methods Study Population Patients Were Recruitedmentioning

confidence: 99%

mentioning

confidence: 99%

Distinct clinical and metabolic deficits in PCA and AD are not related to amyloid distribution

Rosenbloom¹,

Alkalay²,

Agarwal³

et al. 2011

Neurology

118

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“…The subgroups of AD patients were classified based on a determined cut-off of 65 years of age at onset, based on previous studies comparing features of EOAD and LOAD patients (Kemp et al, 2003;Kim et al, 2005;Shiino et al, 2006;Frisoni et al, 2007;Rabinovici et al, 2010;Canu et al, 2012;Sa et al, 2012;Smits et al, 2012;Cho et al, 2013), as well as on clinical grounds (Amaducci et al, 1986). This cut-off is also used in the DSM-IV TR nomenclature to specify subtypes (American Psychiatric Association, 2000).…”

Section: Subjectsmentioning

confidence: 99%

Early-onset and late-onset Alzheimer's disease are associated with distinct patterns of memory impairment

Joubert

Gour

Guedj

et al. 2016

Cortex

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The goal of this study was to investigate the specific patterns of memory breakdown in patients suffering from early-onset Alzheimer's disease (EOAD) and late-onset Alzheimer's disease (LOAD). Twenty EOAD patients, twenty LOAD patients, twenty matched younger controls, and twenty matched older controls participated in this study.All participants underwent a detailed neuropsychological assessment, an MRI scan, an FDG-PET scan, and AD patients had biomarkers as supporting evidence of both amyloïdopathy and neuronal injury. Results of the neuropsychological assessment showed that both EOAD and LOAD groups were impaired in the domains of memory, executive functions, language, praxis, and visuoconstructional abilities, when compared to their respective control groups. EOAD and LOAD groups, however, showed distinct patterns of memory impairment. Even though both groups were similarly affected on measures of episodic, short term and working memory, in contrast semantic memory was significantly more impaired in LOAD than in EOAD patients. The EOAD group was not more affected than the LOAD group in any memory domain. EOAD patients, however, showed significantly poorer performance in other cognitive domains including executive functions and visuoconstructional abilities. A more detailed analysis of the pattern of semantic memory performance among patient groups revealed that the LOAD was more profoundly impaired, in tasks of both spontaneous recall and semantic recognition.Voxel-Based Morphometry (VBM) analyses showed that impaired semantic performance in patients was associated with reduced gray matter volume in the anterior temporal lobe region, while PET-FDG analyses revealed that poorer semantic performance was associated with greater hypometabolism in the left temporoparietal region, both areas reflecting key regions of the semantic network. Results of this study indicate that EOAD and LOAD patients present with distinct patterns of memory impairment, and that a genuine semantic impairment may represent one of the clinical hallmarks of LOAD.

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“…26 Brain areas showing increased PIB uptake do not completely overlap typical sites of neurodegeneration; PIB binding does not increase with time 27 ; not all patients with positive PIB PET develop AD; and the mechanism by which ␤ amyloid leads to neurofibrillary tangle formation, synaptic loss, and cell death, characteristic of pathology is still not clear. 28 In addition, in a comparison of early-onset (younger than 65 years) and late-onset (older than 65 years) AD, there was no difference in the extent or severity of PIB uptake, but metabolic defects on FDG-PET were, as expected, greater in the early-onset group.…”

Section: Molecular Imaging With Amyloid-specific Pet Ligandsmentioning

confidence: 99%

“…28 In addition, in a comparison of early-onset (younger than 65 years) and late-onset (older than 65 years) AD, there was no difference in the extent or severity of PIB uptake, but metabolic defects on FDG-PET were, as expected, greater in the early-onset group. 26 Positive PIB PET correlates with CSF amyloid ␤ 42 , but there is poor correlation of PIB PET with hippocampal volume. 29 While both (neurofibrillary tangles) and amyloid (plaques) have been regarded as hallmarks of AD, it is evident that these act on the brain, and, therefore, influence brain imaging at REVIEW ARTICLE different phases of disease evolution.…”

Section: Molecular Imaging With Amyloid-specific Pet Ligandsmentioning

confidence: 99%

Imaging Approaches for Dementia

Murray

2011

AJNR Am J Neuroradiol

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SUMMARY:Brain imaging has progressed from exclusion of rare treatable mass lesions to a specific antemortem diagnosis. MR imagingϪderived hippocampal atrophy and WMH are regarded as imaging biomarkers of AD and CVD respectively. Abnormal FP-CIT SPECT or cardiac iodobenzamide SPECT is a useful supportive imaging feature in the diagnosis of DLB. Frontal and/or anterior temporal atrophy and anterior defects on molecular imaging with FDG-PET or perfusion SPECT are characteristic of FTDs. Whole-body FDG-PET may be helpful in patients with rapidly progressing "autoimmune dementias," and FLAIR and DWI are indicated in suspected CJD. A major role of imaging is in the development of new drugs and less costly biomarkers.ABBREVIATIONS: apoE ϭ apolipoprotein E; APP ϭ amyloid precursor protein; bvFTD ϭ behavior variant frontotemporal dementia; CJD ϭ Creutzfeldt-Jacob disease; CVD ϭ cerebrovascular disease; DLB ϭ dementia with Lewy bodies; FP-CIT ϭ iodine-123-␤-carbomethoxy-3 ␤-(4-iodophenyltropane) fluoropropyl; FTD ϭ frontotemporal dementia; MCI ϭ mild cognitive impairment; PD ϭ Parkinson disease; rCBF ϭ regional cerebral blood flow; sCJD ϭ sporadic Creutzfeldt-Jacob disease; TDP ϭ TAR deoxyribonucleic acidϪbinding protein 43; VBM ϭ voxel-based morphometry; vCJD ϭ variant Creutzfeldt-Jacob disease; WMH ϭ white matter hyperintensities

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Increased metabolic vulnerability in early-onset Alzheimer’s disease is not related to amyloid burden

Cited by 246 publications

References 99 publications

Distinct clinical and metabolic deficits in PCA and AD are not related to amyloid distribution

Distinct clinical and metabolic deficits in PCA and AD are not related to amyloid distribution

Early-onset and late-onset Alzheimer's disease are associated with distinct patterns of memory impairment

Imaging Approaches for Dementia

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