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Published in: The International Journal of Cardiovascular Imaging 1/2016

01-01-2016 | Original Paper

High resolution FDG-microPET of carotid atherosclerosis: plaque components underlying enhanced FDG uptake

Authors: Jin Liu, William S. Kerwin, James H. Caldwell, Marina S. Ferguson, Daniel S. Hippe, Adam M. Alessio, Vanesa Martinez-Malo, Kristi Pimentel, Robert S. Miyaoka, Ted R. Kohler, Thomas S. Hatsukami, Chun Yuan

Published in: The International Journal of Cardiovascular Imaging | Issue 1/2016

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Abstract

This study sought to discover which atherosclerotic plaque components co-localize with enhanced [18F]-fluorodeoxyglucose (FDG) uptake in carotid positron emission tomography (PET) images. Although in vivo PET currently lacks the resolution, high-resolution ex vivo FDG-microPET with histology validation of excised carotid plaque might accomplish this goal. Thirteen patients were injected with FDG before carotid endarterectomy. After excision, the plaque specimens were scanned by microPET and magnetic resonance imaging, and then serially sectioned for histological analysis. Two analyses were performed using generalized linear mixed models: (1) a PET-driven analysis which sampled high and low FDG uptake areas from PET images to identify their components in matched histology specimens; and (2) a histology-driven analysis where specific plaque components were selected and matched to corresponding PET images. In the PET-driven analysis, regions of high FDG uptake were more likely to contain inflammatory cells (p < 0.001) and neovasculature (p = 0.008) than regions of low FDG uptake. In the histology-driven analysis, regions with inflammatory cells (p = 0.001) and regions with loose extracellular matrix (p = 0.001) were associated with enhanced FDG uptake. Furthermore, areas of complex inflammatory cell infiltrate (co-localized macrophages, lymphocytes and foam cells) had the highest FDG uptake among inflammatory subgroups (p < 0.001). In conclusion, in carotid plaque, regions of inflammatory cell infiltrate, particularly complex one, co-localized with enhanced FDG uptake in high-resolution FDG-microPET images. Loose extracellular matrix and areas containing neovasculature also produced FDG signal. This study points to the potential ability of FDG-PET to detect the cellular components of the vulnerable plaque.
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Metadata
Title
High resolution FDG-microPET of carotid atherosclerosis: plaque components underlying enhanced FDG uptake
Authors
Jin Liu
William S. Kerwin
James H. Caldwell
Marina S. Ferguson
Daniel S. Hippe
Adam M. Alessio
Vanesa Martinez-Malo
Kristi Pimentel
Robert S. Miyaoka
Ted R. Kohler
Thomas S. Hatsukami
Chun Yuan
Publication date
01-01-2016
Publisher
Springer Netherlands
Published in
The International Journal of Cardiovascular Imaging / Issue 1/2016
Print ISSN: 1569-5794
Electronic ISSN: 1875-8312
DOI
https://doi.org/10.1007/s10554-015-0739-2

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