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Metabolic syndrome, fatty liver, and artificial intelligence-based epicardial adipose tissue measures predict long-term risk of cardiac events: a prospective study

机译:代谢综合征,脂肪肝和基于人工智能的外膜脂肪组织措施预测心脏事件的长期风险:一个前瞻性研究

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We sought to evaluate the association of metabolic syndrome (MetS) and computed tomography (CT)-derived cardiometabolic biomarkers (non-alcoholic fatty liver disease [NAFLD] and epicardial adipose tissue [EAT] measures) with long-term risk of major adverse cardiovascular events (MACE) in asymptomatic individuals. This was a post-hoc analysis of the prospective EISNER (Early-Identification of Subclinical Atherosclerosis by Noninvasive Imaging Research) study of participants who underwent baseline coronary artery calcium (CAC) scoring CT and 14-year follow-up for MACE (myocardial infarction, late revascularization, or cardiac death). EAT volume (cm3) and attenuation (Hounsfield units [HU]) were quantified from CT using fully automated deep learning software (?30?s per case). NAFLD was defined as liver-to-spleen attenuation ratio ?1.0 and/or average liver attenuation ?40 HU. In the final population of 2068 participants (59% males, 56?±?9 years), those with MetS (n?=?280;13.5%) had a greater prevalence of NAFLD (26.0% vs. 9.9%), higher EAT volume (114.1 cm3 vs. 73.7 cm3), and lower EAT attenuation (?76.9 HU vs. ?73.4 HU; all p??0.001) compared to those without MetS. At 14?±?3 years, MACE occurred in 223 (10.8%) participants. In multivariable Cox regression, MetS was associated with increased risk of MACE (HR 1.58 [95% CI 1.10–2.27], p?=?0.01) independently of CAC score; however, not after adjustment for EAT measures (p?=?0.27). In a separate Cox analysis, NAFLD predicted MACE (HR 1.78 [95% CI 1.21–2.61], p?=?0.003) independently of MetS, CAC score, and EAT measures. Addition of EAT volume to current risk assessment tools resulted in significant net reclassification improvement for MACE (22% over ASCVD risk score; 17% over ASCVD risk score plus CAC score). MetS, NAFLD, and artificial intelligence-based EAT measures predict long-term MACE risk in asymptomatic individuals. Imaging biomarkers of cardiometabolic disease have the potential for integration into routine reporting of CAC scoring CT to enhance cardiovascular risk stratification. Trial registration NCT00927693.
机译:我们试图评估代谢综合征(METS)和计算机断层扫描(CT)的心脏素质生物标志物(非酒精性脂肪肝疾病[NAFLD]和心外膜脂肪组织[吃]措施)的关联,具有主要不良心血管的长期风险无症状个人的事件(钉子)。这是对前瞻性eisner的后期分析分析(未经侵入性影像学研究的早期鉴定亚临床动脉粥样硬化)研究,接受基线冠状动脉钙(CAC)评分CT和14年的术语术(心肌梗死,晚期血运重建,或心脏死亡)。吃体积(cm3)和衰减(Hounsfield单位[hu])从CT使用全自动深度学习软件量化(&每个案例)量化。 NAFLD被定义为肝脏到脾脏衰减比率& 1.0和/或平均肝脏衰减&?40 hu。在2068名参与者的最终人口(59%的男性,56次?体积(114.1 cm3 vs. 73.7 cm3),较低的饮食衰减(Δ76.9u与α73.4hu;所有p?& 0.001)与没有mets的那些相比。在14?±3年后,Mace发生在223名(10.8%)参与者中。在多变量的Cox回归中,Mets与CAC评分的术风险增加(HR 1.58 [95%CI 1.10-2.27],p?= 0.01)相关;但是,没有经过饮食措施调整(p?= 0.27)。在单独的COX分析中,NAFLD预测术(HR 1.78 [95%CI 1.21-2.61],P?= 0.003)独立于METS,CAC评分和吃措施。为当前风险评估工具添加额外的卷导致MACE的净重新分类改善(ASCVD风险评分22%; ASCVD风险得分为CAC得分,17%。 Mets,Nafld和基于人工智能的饮食措施预测无症状的人的长期坐线风险。心肌素疾病的成像生物标志物有可能融入CAC评分CT的常规报告,以提高心血管风险分层。试验登记NCT00927693。

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