Early detection of amyloid load using 18F-florbetaben PET [electronic resource]

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Tác giả:

Ngôn ngữ: eng

Ký hiệu phân loại: 617.5 Regional medicine Regional surgery

Thông tin xuất bản: Washington, D.C. : Oak Ridge, Tenn. : United States. Dept. of Energy. Office of Science ; Distributed by the Office of Scientific and Technical Information, U.S. Dept. of Energy, 2021

Mô tả vật lý: Size: Article No. 67 : , digital, PDF file.

Bộ sưu tập: Metadata

ID: 259721

 A low amount and extent of A? deposition at early stages of Alzheimer?s disease (AD) may limit the use of previously developed pathology-proven composite SUVR cutoffs. This study aims to characterize the population with earliest abnormal A? accumulation using 18F-florbetaben PET. Quantitative thresholds for the early (SUVR<
 sub>
 early<
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 ) and established (SUVR<
 sub>
 estab<
 /sub>
 ) A? deposition were developed, and the topography of early A? deposition was assessed. Subsequently, A? accumulation over time, progression from mild cognitive impairment (MCI) to AD dementia, and tau deposition were assessed in subjects with early and established A? deposition. The study population consisted of 686 subjects (n = 287 (cognitively normal healthy controls), n = 166 (subjects with subjective cognitive decline (SCD)), n = 129 (subjects with MCI), and n = 101 (subjects with AD dementia)). Three categories in the A?-deposition continuum were defined based on the developed SUVR cutoffs: A?-negative subjects, subjects with early A? deposition (?gray zone?), and subjects with established A? pathology. SUVR using the whole cerebellum as the reference region and centiloid (CL) cutoffs for early and established amyloid pathology were 1.10 (13.5 CL) and 1.24 (35.7 CL), respectively. Cingulate cortices and precuneus, frontal, and inferior lateral temporal cortices were the regions showing the initial pathological tracer retention. Subjects in the ?gray zone? or with established A? pathology accumulated more amyloid over time than A?-negative subjects. After a 4-year clinical follow-up, none of the A?-negative or the gray zone subjects progressed to AD dementia while 91% of the MCI subjects with established A? pathology progressed. Tau deposition was infrequent in those subjects without established A? pathology. This study supports the utility of using two cutoffs for amyloid PET abnormality defining a ?gray zone?: a lower cutoff of 13.5 CL indicating emerging A? pathology and a higher cutoff of 35.7 CL where amyloid burden levels correspond to established neuropathology findings. These cutoffs define a subset of subjects characterized by pre-AD dementia levels of amyloid burden that precede other biomarkers such as tau deposition or clinical symptoms and accelerated amyloid accumulation. The determination of different amyloid loads, particularly low amyloid levels, is useful in determining who will eventually progress to dementia. Quantitation of amyloid provides a sensitive measure in these low-load cases and may help to identify a group of subjects most likely to benefit from intervention.
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