PIB is a non-specific imaging marker of amyloid-beta (A ) peptide-related cerebral amyloidosis

Lockhart, Andrew; Lamb, Jonathan R.; Osredkar, Tracy; Sue, Lucia I.; Joyce, Jeffrey N.; Ye, L.; Libri, Vincenzo; Leppert, David; Beach, Thomas G.

doi:10.1093/brain/awm191

Cited by 287 publications

(270 citation statements)

References 49 publications

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“…In the absence of congophilic angiopathy, perivascular accumulation of PiB has been previously reported as representing either a nonspecific interaction (27,28) or an artifact (28).…”

Section: Discussionmentioning

confidence: 99%

Characterization of PiB Binding to White Matter in Alzheimer Disease and Other Dementias

Fodero‐Tavoletti¹,

Rowe²,

McLean³

et al. 2009

J Nucl Med

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11 C-Pittsburgh Compound B ( 11 C-PiB) PET has demonstrated significantly higher PiB retention in the gray matter of Alzheimer disease (AD) patients than in healthy controls (HCs). PiB is similarly retained within the white matter of HC and AD brains. Although the specificity of PiB for Ab plaques in gray matter has been well described, the nature of PiB binding to white matter remains unclear. In this study, we characterized the binding of PiB to human white matter homogenates. Methods: In vitro binding studies were conducted using 3 H-PiB (0.1-500 nM) and white matter brain homogenates (100 mg) from 3 AD patients and 3 HCs. Nonspecific binding was determined using PiB (1 mM). White matter from the same patients was also analyzed by immunofluorescence/immunohistochemistry (IF/IHC) microscopy and Western blotting for Ab expression. White matter kinetics were also characterized in vivo through 11 C-PiB PET studies in 27 HCs and 34 patients with dementia. IF/IHC experiments were conducted on 1 postmortem patient with dementia, to compare with the 11 C-PiB distribution volume ratio data acquired 23 mo earlier. Results: In vitro saturation studies indicated that 3 HPiB binds nonspecifically to white matter brain homogenates. PiB fluorescence staining of AD and HC brain sections was consistent with absence of Ab in IHC staining. Higher gray matterto-white matter ratios were observed in IHC images than in 11 C-PiB PET images. Conclusion: These studies suggest that PiB binding to white matter is mainly nonsaturable and nonspecific and that PiB retention in the 11 C-PiB PET studies is largely attributable to slower PiB white matter kinetics.

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“…In the absence of congophilic angiopathy, perivascular accumulation of PiB has been previously reported as representing either a nonspecific interaction (27,28) or an artifact (28).…”

Section: Discussionmentioning

confidence: 99%

Characterization of PiB Binding to White Matter in Alzheimer Disease and Other Dementias

Fodero‐Tavoletti¹,

Rowe²,

McLean³

et al. 2009

J Nucl Med

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“…Nevertheless, the histological hallmarks of AD pathology, comprising amyloid plaques and neurofibrillary tangles, are known to occur up to 10 to 20 years before the objective detection of cognitive decline [1]. Recently, positron emission tomography (PET) using Pittsburgh compound B (PiB) has been introduced as a diagnostic tool to detect cerebral amyloid in vivo [2][3][4][5][6][7][8]. The major disadvantages of PiB-PET are the need to use a radioactive tracer, the relative scarcity of institutions that can perform such scans because of the requirement for an onsite cyclotron, the inability to acquire anatomic and functional information in the brain during the same examination, and the greater chance of false positives, making interpretation of PiB-PET scans more difficult, especially in the elderly, which hampers the use of this method as a diagnostic tool in the elderly [9].…”

Section: Introductionmentioning

confidence: 99%

Cortical phase changes in Alzheimer's disease at 7T MRI: A novel imaging marker

Rooden

Versluis

Liem

et al. 2013

Alzheimer's & Dementia

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Background: Postmortem studies have indicated the potential of high-field magnetic resonance imaging (MRI) to visualize amyloid depositions in the cerebral cortex. The aim of this study is to test this hypothesis in patients with Alzheimer's disease (AD). Methods: T2*-weighted MRI was performed in 16 AD patients and 15 control subjects. All magnetic resonance images were scored qualitatively by visual assessment, and quantitatively by measuring phase shifts in the cortical gray matter and hippocampus. Statistical analysis was performed to assess differences between groups.Results: Patients with AD demonstrated an increased phase shift in the cortex in the temporoparietal, frontal, and parietal regions (P , .005), and this was associated with individual Mini-Mental State Examination scores (r 5 20.54, P , .05). Conclusion: Increased cortical phase shift in AD patients demonstrated on 7-tesla T2*-weighted MRI is a potential new biomarker for AD, which may reflect amyloid pathology in the early stages.

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“…Importantly, on the basis of concentrations achieved during PET studies, cortical retention of 11 C-PIB has been shown to reflect Aβ load as opposed to Lewy bodies or tau pathology (Fodero-Tavoletti et al, 2007;Lockhart et al, 2007;Ikonomovic et al, 2008). In addition to accelerating current understanding of cerebral amyloidosis and advancing detection of AD pathology to an earlier stage (Klunk et al, 2004;Mintun et al, 2006;Rowe et al, 2007;Cohen et al, 2012), 11 C-PIB has contributed to improvements in the differential diagnosis of neurodegenerative diseases (Ng et al, 2007;Rabinovici et al, 2007;Rowe et al, 2007).…”

Section: First Generation Of Amyloid Probes: 11 C Pittsburgh Compound Bmentioning

confidence: 99%

Imaging biomarkers for amyloid: a new generation of probes and what lies ahead

Leuzy

Zimmer

Bhat

et al. 2014

Int. Psychogeriatr.

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Since the original 1984 criteria for Alzheimer's disease (AD), put forth by a work group jointly established by the National Institute of Neurological and Communicative Disorders and Stroke (NINCDS) and the Alzheimer's Disease and Related Disorders Association (ADRDA) (McKhann et al., 1984), important advances have occurred in our ability to detect AD pathophysiology, with the incorporation of biomarkers – defined as anatomic, biochemical, or physiologic parameters that provide in vivo evidence of AD neuropathology (Cummings, 2011) – that can improve the certainty of AD diagnosis. Use of imaging biomarkers such as positron emission tomography (PET) with amyloid ligands, particularly in asymptomatic and pre-dementia stages of AD, however, has been the subject of debate (Dubois et al., 2013), with arguments both for and against the biomarker driven diagnosis of AD.

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PIB is a non-specific imaging marker of amyloid-beta (A ) peptide-related cerebral amyloidosis

Cited by 287 publications

References 49 publications

Characterization of PiB Binding to White Matter in Alzheimer Disease and Other Dementias

Characterization of PiB Binding to White Matter in Alzheimer Disease and Other Dementias

Cortical phase changes in Alzheimer's disease at 7T MRI: A novel imaging marker

Imaging biomarkers for amyloid: a new generation of probes and what lies ahead

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