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血管壁的氟代脱氧葡萄糖摄取是否应根据动脉粥样硬化负担程度进行调整?

Should vascular wall F-FDG uptake be adjusted for the extent of atherosclerotic burden?

作者信息

Lensen Karel-Jan D F, Voskuyl Alexandre E, Comans Emile F I, van der Laken Conny J, Boellaard Ronald, Smulders Yvo M

机构信息

Department of Internal Medicine, Amsterdam University Medical Center, Boelelaan, Amsterdam, The Netherlands.

Department of Internal Medicine, University Medical Center Groningen, PO Box 30.001, 9700 RB, Groningen, The Netherlands.

出版信息

Int J Cardiovasc Imaging. 2020 Mar;36(3):545-551. doi: 10.1007/s10554-019-01744-0. Epub 2020 Jan 2.

Abstract

Vascular wall F-FDG uptake is often used as a surrogate marker of atherosclerotic plaque inflammation. A potential caveat is that vascular wall F-FDG uptake is higher simply because more atherosclerosis is present. To determine if the degree of inflammation is high or low relative to the extent of atherosclerosis, vascular wall F-FDG uptake may require statistical adjustment for a non-inflammatory marker reflecting the extent of atherosclerosis, e.g. calcification. Adjustments is probably needed if (1) vascular wall F-FDG uptake correlates sufficiently strongly with arterial calcification and (2) adjustment for extent of calcification affects determinants of vascular F-FDG uptake. This study addresses these questions. F-FDG PET/low-dose-CT scans of 99 patients were used. Cardiovascular risk factors were assessed and PET/CT scans were analysed for standardized F-FDG uptake values and calcification. ANOVA was used to establish the association between vascular F-FDG uptake and calcification. Multiple linear regression (with and without calcification as independent variable) was used to show whether determinants of vascular F-FDG uptake were affected by the degree of calcification. F-FDG uptake was related to increased calcification in the aortic arch, descending and abdominal aorta. However, F-FDG uptake showed considerable overlap between categories of calcification. Age and body mass index were main determinants of vascular F-FDG uptake. In multiple regression analyses, most standardized beta coefficients of these determinants were not affected by adjustment for the degree of calcification. Although vascular F-FDG uptake is related to total atherosclerotic burden, as reflected by vascular calcification, the association is weak and unlikely to affect the identification of determinants of atherosclerotic inflammation implicating no need for adjustment in future studies.

摘要

血管壁F-FDG摄取常被用作动脉粥样硬化斑块炎症的替代标志物。一个潜在的问题是,血管壁F-FDG摄取较高仅仅是因为存在更多的动脉粥样硬化。为了确定相对于动脉粥样硬化程度而言炎症程度是高还是低,血管壁F-FDG摄取可能需要针对反映动脉粥样硬化程度的非炎症标志物(如钙化)进行统计调整。如果(1)血管壁F-FDG摄取与动脉钙化的相关性足够强,且(2)钙化程度的调整影响血管F-FDG摄取的决定因素,则可能需要进行调整。本研究探讨了这些问题。使用了99例患者的F-FDG PET/低剂量CT扫描。评估了心血管危险因素,并对PET/CT扫描分析了标准化的F-FDG摄取值和钙化情况。采用方差分析来确定血管F-FDG摄取与钙化之间的关联。使用多元线性回归(以钙化与否作为自变量)来显示血管F-FDG摄取的决定因素是否受钙化程度的影响。F-FDG摄取与主动脉弓、降主动脉和腹主动脉钙化增加有关。然而,F-FDG摄取在钙化类别之间存在相当大的重叠。年龄和体重指数是血管F-FDG摄取的主要决定因素。在多元回归分析中,这些决定因素的大多数标准化β系数不受钙化程度调整的影响。尽管血管F-FDG摄取与血管钙化所反映的总动脉粥样硬化负担有关,但这种关联较弱,不太可能影响动脉粥样硬化炎症决定因素的识别,这意味着未来研究无需进行调整。

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