心房18f -氟脱氧葡萄糖摄取增加:心房颤动患者心房炎症增加的证据?

O. Nakamura, C. Goetz, P. Meyer, T. Arentz, A. Jadidi
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引用次数: 0

摘要

资金来源类型:无。心房炎症和纤维化重构是心房心肌病的病理生理学基础,它与心房颤动(AF)和心房扑动(AFL)的发展有关。18f -氟脱氧葡萄糖正电子发射断层扫描/计算机断层扫描(18F-FDG-PET/CT)已被用于检测炎症过程。最近的研究显示房颤患者心房中fdg摄取增加,但在诊断为心脏结节病并发心室炎症的患者中也是如此。本研究旨在评估PET/CT在专用心脏FDG-PET/CT人群中检测和量化心房炎症(fdg摄取)程度的能力。我们调查了101例疑似结节病的患者(57±12岁,72%男性),他们接受了18F-FDG PET/CT扫描,并进行了专门的心脏特异性准备(肝素输注,禁食12小时,高脂低碳水化合物饮食)。我们排除了活动性室性心脏结节病患者或接受高剂量免疫抑制治疗的患者(强的松龙≥20mg/天或强的松龙联合其他免疫治疗,如甲氨蝶呤)。测定心房心肌最大标准化摄取值(SUVmax)和血池平均标准化摄取值(SUVmean),计算心房心肌SUVmax与血池SUVmean的靶本比(TBR)。所有的医疗记录、心律失常类型的心电图数据和系统性结节病的诊断(没有心室受累)被用于分析。结节病是根据日本卫生和福利部2006年制定的标准诊断的。根据有无心律失常和系统性结节病进行分类,比较各组TBR。房颤或AFL发生率为30/101。101例患者中有37例发现系统性结节病。已知AF/AFL患者与无AF/AFL患者相比,心房组织内TBR显著增加:(中位数:1.26,第1 -3四分位数:1.20-1.33)vs(中位数:1.22,第1 -3四分位数:1.14-1.25;P = 0.004;图A)。一贯观察到心律失常相关的心房炎症,而不考虑是否伴有系统性结节病(图B)。经TBR鉴定,同时患有心房心律失常和系统性结节病的患者心房炎症水平最高(图B)。心房颤动或扑动的发展与心房fdg摄取增加相关,fdg摄取是心房炎症的代谢标志物。心房炎症的水平进一步提高了额外的系统性结节病的存在。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Increased 18F-fluorodeoxyglucose uptake in the cardiac atria: an evidence for increased atrial inflammation in patients with atrial fibrillation?
Type of funding sources: None. Atrial inflammation and fibrotic remodelling underlie the pathophysiology of atrial cardiomyopathy, which is associated with the development of atrial fibrillation (AF) and atrial flutter (AFL). 18F-fluorodeoxyglucose positron emission tomography/computed tomography (18F-FDG-PET/CT) has been used to detect inflammatory processes. Recent studies have revealed an increased FDG-uptake in the atria of patients with AF, but also in patients with diagnosis of cardiac sarcoidosis with ventricular inflammation. This study aimed to assess the capability of PET/CT to detect and quantify the degree of atrial inflammation (FDG-uptake) in a population with dedicated cardiac FDG-PET/CT. We investigated 101 patients suspected of sarcoidosis (57±12 years, 72% male) who underwent 18F-FDG PET/CT scan with dedicated cardiac specific preparation (heparin infusion, 12 hours fasting, and high-fat low-carbohydrate diet). We excluded patients with active ventricular cardiac sarcoidosis or undergoing high-dose immunosuppressive therapy (prednisolone ≥20mg/day or prednisolone combined with other immunotherapy like methotrexate). We measured the maximum standardized uptake value (SUVmax) in atrial myocardium and mean standardized uptake value (SUVmean) in blood pool and calculated the target-to-background ratio (TBR) of SUVmax in atrial myocardium to SUVmean in blood pool. All medical records, ECG data on arrhythmia type and diagnosis of systemic sarcoidosis (with absence of ventricular involvement) were used for the analysis. Sarcoidosis was diagnosed based on the criteria established in 2006 by the Japanese Ministry of Health and Welfare. The collected data were sorted according to presence of arrhythmia and systemic sarcoidosis and TBR of each group were compared. AF or AFL was found in 30/101 patients. Systemic sarcoidosis was found in 37/101 patients. Patients with known AF/AFL had significantly increased TBR within the atrial tissue compared to those without AF/AFL: (median: 1.26, 1st-3rd quartile: 1.20-1.33) versus (median: 1.22, 1st-3rd quartile: 1.14-1.25; p = 0.004; figure A). Arrhythmia-associated atrial inflammation was consistently observed, independently of presence of concomitant systemic sarcoidosis (figure B). Patients with both atrial arrhythmias and systemic sarcoidosis had the highest atrial inflammation level, as identified by TBR (figure B). Development of atrial fibrillation or flutter is associated with an increased atrial FDG-uptake as metabolic marker of atrial inflammation. The level of atrial inflammation is further enhanced by additional presence of systemic sarcoidosis.
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