Cardiology Division, Cardiovascular Research Center, Massachusetts General Hospital, Harvard Medical School, Boston, MA (C.W.K., G.Q., F.A.J.).
Department of Cardiovascular Medicine, Masonic Medical Research Institute, Utica, NY (C.W.K.).
Circ Cardiovasc Imaging. 2021 Mar;14(3):e011898. doi: 10.1161/CIRCIMAGING.120.011898. Epub 2021 Mar 16.
The postthrombotic syndrome is a common, often morbid sequela of venous thrombosis (VT) that arises from thrombus persistence and inflammatory scarring of juxtaposed vein walls and valves. Noninvasive F-fluorodeoxyglucose (FDG) positron emission tomography/computed tomography (PET/CT) imaging can measure neutrophil inflammation in VT. Here, we hypothesized (1) early fluorodeoxyglucose positron emission tomography/computed tomography (FDG-PET/CT) VT inflammation can predict subsequent vein wall scarring (VWS) and (2) statin therapy can reduce FDG-PET VT inflammation and subsequent VWS.
C57BL/6J mice (n=75) underwent induction of stasis-induced VT of the inferior vena cava or jugular vein. Inferior vena cava VT mice (n=44) were randomized to daily oral rosuvastatin 5 mg/kg or saline starting at day -1. Subgroups of mice then underwent FDG-PET/CT 2 days after VT induction. On day 14, a subset of mice was euthanized, and VWS was assessed via histology. In vitro studies were further performed on bone marrow-derived neutrophils.
Statin therapy reduced early day 2 FDG-PET VT inflammation, thrombus neutrophil influx, and plasma IL (interleukin)-6 levels. At day 14, statin therapy reduced VWS but did not affect day 2 thrombus mass, cholesterol, or white blood counts, nor reduce day 2 glucose transporter 1 or myeloperoxidase expression in thrombus or in isolated neutrophils. In survival studies, the day 2 FDG-PET VT inflammation signal as measured by mean and maximum standardized uptake values predicted the extent of day 14 VWS (area under the receiver operating characteristic curve =0.82) with a strong correlation coefficient () of =0.73 and =0.74, respectively. Mediation analyses revealed that 40% of the statin-induced VWS reduction was mediated by reductions in VT inflammation as quantified by FDG-PET.
Early noninvasive FDG-PET/CT imaging of VT inflammation predicts the magnitude of subsequent VWS and may provide a new translatable approach to identify individuals at risk for postthrombotic syndrome and to assess anti-inflammatory postthrombotic syndrome therapies, such as statins.
血栓后综合征是静脉血栓形成(VT)的常见且常导致病态的后遗症,它源于血栓的持续存在以及毗邻静脉壁和瓣膜的炎症性瘢痕形成。非侵入性 F-氟脱氧葡萄糖(FDG)正电子发射断层扫描/计算机断层扫描(PET/CT)成像可测量 VT 中的中性粒细胞炎症。在这里,我们假设(1)早期 FDG-PET/CT 静脉血栓形成炎症可预测随后的静脉壁瘢痕形成(VWS),以及(2)他汀类药物治疗可减少 FDG-PET VT 炎症和随后的 VWS。
C57BL/6J 小鼠(n=75)接受下腔静脉或颈静脉淤滞诱导的 VT 形成。下腔静脉 VT 小鼠(n=44)从-1 天开始每天接受口服瑞舒伐他汀 5mg/kg 或盐水。然后,将小鼠随机分组进行 FDG-PET/CT 检查,检查时间为 VT 诱导后 2 天。第 14 天,部分小鼠被安乐死,并通过组织学评估 VWS。进一步进行了骨髓来源的中性粒细胞的体外研究。
他汀类药物治疗降低了第 2 天早期 FDG-PET VT 炎症、血栓中性粒细胞浸润和血浆白细胞介素(IL)-6 水平。第 14 天,他汀类药物治疗降低了 VWS,但并未影响第 2 天血栓质量、胆固醇或白细胞计数,也未降低第 2 天葡萄糖转运蛋白 1 或髓过氧化物酶在血栓或分离的中性粒细胞中的表达。在生存研究中,通过平均和最大标准摄取值测量的第 2 天 FDG-PET VT 炎症信号预测了第 14 天 VWS 的程度(接受者操作特征曲线下面积=0.82),具有强相关系数()为=0.73 和=0.74。中介分析表明,他汀类药物诱导的 VWS 减少有 40%是通过 FDG-PET 量化的 VT 炎症减少介导的。
早期非侵入性 FDG-PET/CT 静脉血栓形成炎症成像可预测随后 VWS 的严重程度,并可能为识别易患血栓后综合征的个体以及评估他汀类药物等抗炎性血栓后综合征治疗方法提供一种新的可转化方法。
