Diagnostic potential of soluble ST2 and D-dimer for Stanford Type B aortic dissection and intramural aortic hematoma

IF 2.9 4区 医学 Q2 PERIPHERAL VASCULAR DISEASE Microvascular research Pub Date : 2023-11-03 DOI:10.1016/j.mvr.2023.104623
Qian Zhu , Lei Wang , Chao Dai , Yonghua Zhang , Pengpeng Han , Yongxiang Huang , Huan Liu , Lixin Wang
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Abstract

Objective

Type B aortic dissection (TBAD) and intramural aortic hematoma (IMH) are common manifestations of Acute Aortic Syndrome (AAS), exhibiting overlapping clinical features. The timely and accurate diagnosis and differentiation between TBAD and IMH are critical for appropriate management. Tumorigenicity 2 (sST2) and D-dimer have been shown to elevate levels in both TBAD and IMH, making them valuable as “rule-out” markers. Hence, we aimed to assess the diagnostic utility of sST2 and D-dimer in distinguishing TBAD from IMH.

Methods

In this retrospective study, we analyzed serum levels of sST2 and D-dimer in 182 AAS patients, comprising 90 TBAD cases, 92 IMH cases, and 90 non-AAS cases. Serial measurements were taken at 1 h, 6 h, 12 h, 24 h, and 72 h post-admission. Comparative analyses were conducted between TBAD and non-AAS cases, IMH and non-AAS cases, and TBAD and IMH cases. Receiver operating characteristic (ROC) curve analysis was performed to evaluate the diagnostic accuracy of sST2 and D-dimer in identifying TBAD or IMH cases.

Results

Both TBAD and IMH patients displayed elevated levels of sST2 and D-dimer compared to non-AAS cases. Notably, sST2 levels were significantly higher in TBAD patients than in IMH patients, whereas D-dimer levels exhibited moderate differences. TBAD patients tended to exhibit elevated levels of either sST2 or D-dimer, with a modest correlation between the two (Pearson correlation coefficient = 0.3614). In contrast, IMH patients showed elevations in both markers, with a positive correlation between them (Pearson correlation coefficient = 0.6814). The ROC analysis revealed that both sST2 (AUC, 0.657; 95 % CI, 0.552–0.753; cutoff value, 27.54 ng/ml) and D-dimer (AUC, 0.695; 95 % CI, 0.591–0.787, cutoff value, 1.215 ng/ml) demonstrated favorable diagnostic performance for TBAD. sST2 exhibited a sensitivity of 80.92 % and a specificity of 75.00 %, while D-dimer showed a sensitivity of 80.92 % and a specificity of 75.00 %. For the diagnosis of IMH, the combined assessment of sST2 and D-dimer (AUC, 0.674; 95 % CI, 0.599–0.768; sensitivity, 69.20 %; specificity, 80.00 %) proved effective.

Conclusions

Our results indicate that both sST2 and D-dimer show diagnostic potential for TBAD. Elevated levels of either serve as an indicator of TBAD onset. However, concurrent elevation of both markers seems to be indicative of IMH. The combination of increased sST2 and D-dimer levels demonstrates strong diagnostic performance in identifying IMH cases.

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可溶性ST2和D-二聚体对Stanford B型主动脉夹层和壁内主动脉血肿的诊断潜力。
目的:B型主动脉夹层(TBAD)和壁内主动脉血肿(IMH)是急性主动脉综合征(AAS)的常见表现,具有重叠的临床特征。及时准确地诊断和区分TBAD和IMH对于适当的管理至关重要。致瘤性2(sST2)和D-二聚体已被证明可提高TBAD和IMH的水平,使其成为有价值的“排除”标志物。因此,我们旨在评估sST2和D-二聚体在区分TBAD和IMH方面的诊断效用。方法:在这项回顾性研究中,我们分析了182名AAS患者的血清sST2和D-二聚体水平,包括90例TBAD病例、92例IMH病例和90例非AAS病例。在1进行了连续测量 h、 6 h、 12 h、 24 h、 和72 h入院后。对TBAD和非AAS病例、IMH和非AAS病例以及TBAD和IMH病例进行比较分析。进行受试者操作特征(ROC)曲线分析,以评估sST2和D-二聚体在识别TBAD或IMH病例中的诊断准确性。结果:与非AAS病例相比,TBAD和IMH患者的sST2和D-二聚体水平均升高。值得注意的是,TBAD患者的sST2水平显著高于IMH患者,而D-二聚体水平表现出中度差异。TBAD患者往往表现出sST2或D-二聚体水平升高,两者之间存在适度相关性(Pearson相关系数 = 0.3614)。相反,IMH患者的两种标志物均升高,且两者呈正相关(Pearson相关系数 = 0.6814)。ROC分析显示,sST2(AUC,0.657;95 % CI,0.552-0.753;截止值,27.54 ng/ml)和D-二聚体(AUC,0.695;95 % CI,0.591-0.787,截止值,1.215 ng/ml)显示出对TBAD有利的诊断性能。sST2的灵敏度为80.92 % 特异性为75.00 %, D-二聚体的敏感性为80.92 % 特异性为75.00 %. 对于IMH的诊断,sST2和D-二聚体的联合评估(AUC,0.674;95 % CI,0.599-0.768;灵敏度,69.20 %; 特异性,80.00 %) 事实证明是有效的。结论:我们的结果表明,sST2和D-二聚体都显示出对TBAD的诊断潜力。二者中任一者的水平升高可作为TBAD发病的指标。然而,两种标记物同时升高似乎表明IMH。sST2和D-二聚体水平增加的组合在识别IMH病例方面表现出强大的诊断性能。
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来源期刊
Microvascular research
Microvascular research 医学-外周血管病
CiteScore
6.00
自引率
3.20%
发文量
158
审稿时长
43 days
期刊介绍: Microvascular Research is dedicated to the dissemination of fundamental information related to the microvascular field. Full-length articles presenting the results of original research and brief communications are featured. Research Areas include: • Angiogenesis • Biochemistry • Bioengineering • Biomathematics • Biophysics • Cancer • Circulatory homeostasis • Comparative physiology • Drug delivery • Neuropharmacology • Microvascular pathology • Rheology • Tissue Engineering.
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