血管生成素-2 和 D-二聚体为肺动脉高压的临床风险增加了预后信息

Heather L. Clark , Daniel Lachant , Allison N. Light , Deborah Haight , Samia Lopia , Nigel Mackman , R. James White
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引用次数: 0

摘要

背景血栓形成和内皮损伤是肺动脉高压(PAH)的病理特征。我们的目的是评估血液中的内皮功能障碍和凝血标志物是否有助于了解 PAH 的疾病活动、治疗反应和预后。方法我们前瞻性地收集了未经治疗的 PAH 患者(22 人)和有临床指征加强治疗的患者(19 人)的基线和 3 个月随访血液样本。此外,我们还招募了 12 名健康人和临床稳定的 PAH 患者(n = 45)作为对照组,他们在 14 天内采集了两次血液样本。我们生成了无血小板血浆,并测量了 D-二聚体、血管生成素-2、凝血酶时间、可溶性 P-选择素、von Willebrand 因子和血管内皮生长因子。我们用 Reveal Lite 2 评分评估治疗反应(所有患者在两次就诊时都进行了 N 端脑钠肽、6 分钟步行和功能分级评估),并对临床结果进行了为期 3 年的随访。结果血管生成素-2 水平升高,并在有效治疗后下降(Reveal Lite 2 评分下降)。随访时,血管生成素-2水平的持续升高预示着临床事件的发生,甚至能识别出随后发生事件的低风险参与者。PAH 患者的 D-二聚体水平也会升高,但对治疗的反应没有变化。还发现了其他一些内皮和血小板活化异常(包括可溶性 P-选择素升高、von Willebrand 因子升高和血管内皮生长因子升高),但这些异常并未随治疗而改变,也未预测预后。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Angiopoietin-2 and D-dimer add prognostic information to clinical risk in pulmonary arterial hypertension

Background

Thrombosis and endothelial injury are pathologic hallmarks of pulmonary arterial hypertension (PAH). We aimed to evaluate whether markers of endothelial dysfunction and coagulation in the blood would provide insight into disease activity, treatment response, and outcomes in PAH.

Methods

We prospectively collected baseline and 3-month follow-up blood samples from treatment-naïve patients with PAH (n = 22) and those who had a clinical indication to intensify therapy (n = 19). In addition, we recruited 12 healthy people and clinically stable patients with PAH (n = 45) as controls who had 2 blood samples collected twice within 14 days. We generated platelet-free plasma and measured D-dimer, angiopoietin-2, thrombin time, soluble P-selectin, von Willebrand factor, and vascular endothelial growth factor. We assessed treatment response with Reveal Lite 2 scores (all patients had N-terminal-pro-brain natriuretic peptide, 6-minute walk, and functional class assessment at both visits) and followed clinical outcomes for 3 years.

Results

Angiopoietin-2 levels were elevated and fell in response to effective therapy (drop in Reveal Lite 2 score). At follow-up, persistently elevated angiopoietin-2 levels predicted clinical events and even identified low-risk participants who subsequently had events. D-dimer levels were also elevated in patients with PAH but did not change in response to therapy. Several other abnormalities in endothelial and platelet activation were identified (including elevated soluble P-selectin, elevated von Willebrand factor, and elevated vascular endothelial growth factor) but these did not change with treatment or predict outcome.

Conclusions

Angiopoietin-2 and D-dimer are elevated in patients with PAH and may add prognostic information to routine clinical assessment.
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