Pulmonary Hypertension Research Group Centre de Recherche de l'Institut Universitaire de Cardiologie et de Pneumologie de Québec Québec City Québec Canada.
Department of Cardiovascular Medicine Fukushima Medical University Fukushima Japan.
J Am Heart Assoc. 2024 Jun 18;13(12):e032888. doi: 10.1161/JAHA.123.032888. Epub 2024 Jun 14.
Pulmonary arterial hypertension (PAH) ultimately leads to right ventricular failure and premature death. The identification of circulating biomarkers with prognostic utility is considered a priority. As chronic inflammation is recognized as key pathogenic driver, we sought to identify inflammation-related circulating proteins that add incremental value to current risk stratification models for long-term survival in patients with PAH.
Plasma levels of 384 inflammatory proteins were measured with the proximity extension assay technology in patients with PAH (n=60) and controls with normal hemodynamics (n=28). Among these, 51 analytes were significantly overexpressed in the plasma of patients with PAH compared with controls. Cox proportional hazard analyses and C-statistics were performed to assess the prognostic value and the incremental prognostic value of differentially expressed proteins. A panel of 6 proteins (CRIM1 [cysteine rich transmembrane bone morphogenetic protein regulator 1], HGF [hepatocyte growth factor], FSTL3 [follistatin-like 3], PLAUR [plasminogen activator, urokinase receptor], CLSTN2 [calsyntenin 2], SPON1 [spondin 1]) were independently associated with death/lung transplantation at the time of PAH diagnosis after adjustment for the 2015 European Society of Cardiology/European Respiratory Society guidelines, the REVEAL (Registry to Evaluate Early and Long-Term PAH Disease Management) 2.0 risk scores, and the refined 4-strata risk assessment. CRIM1, PLAUR, FSTL3, and SPON1 showed incremental prognostic value on top of the predictive models. As determined by Western blot, FSTL3 and SPON1 were significantly upregulated in the right ventricle of patients with PAH and animal models (monocrotaline-injected and pulmonary artery banding-subjected rats).
In addition to revealing new actors likely involved in cardiopulmonary remodeling in PAH, our screening identified promising circulating biomarkers to improve risk prediction in PAH, which should be externally confirmed.
肺动脉高压(PAH)最终导致右心衰竭和过早死亡。具有预后效用的循环生物标志物的鉴定被认为是当务之急。由于慢性炎症被认为是关键的致病驱动因素,我们试图确定与炎症相关的循环蛋白,这些蛋白可增加当前用于预测 PAH 患者长期生存的风险分层模型的附加值。
采用邻近延伸分析技术检测 60 例 PAH 患者和 28 例血流动力学正常对照者的血浆中 384 种炎症蛋白的水平。其中,51 种分析物在 PAH 患者的血浆中明显过表达。采用 Cox 比例风险分析和 C 统计量评估差异表达蛋白的预后价值和增量预后价值。一组 6 种蛋白(CRIM1[富含半胱氨酸跨膜骨形态发生蛋白调节剂 1]、HGF[肝细胞生长因子]、FSTL3[卵泡抑素样 3]、PLAUR[纤溶酶原激活物,尿激酶受体]、CLSTN2[钙结合蛋白 2]、SPON1[spondin 1])在调整 2015 年欧洲心脏病学会/欧洲呼吸学会指南、REVEAL(评估早期和长期 PAH 疾病管理的登记处)2.0 风险评分和改良的 4 分层风险评估后,与 PAH 诊断时的死亡/肺移植独立相关。CRIM1、PLAUR、FSTL3 和 SPON1 在预测模型的基础上具有增量预后价值。Western blot 结果表明,FSTL3 和 SPON1 在 PAH 患者和动物模型(单硝酸异山梨酯注射和肺动脉结扎大鼠)的右心室中显著上调。
除了揭示可能参与 PAH 心肺重塑的新因子外,我们的筛选还确定了有前途的循环生物标志物,以改善 PAH 的风险预测,这应该得到外部验证。
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