Novel prognostic impact and cell specific role of endocan in patients with coronary artery disease

Author:

Lin Liang-YuORCID,Chang Ting-Ting,Leu Hsin-Bang,Huang Chin-Chou,Wu Tao-Cheng,Chou Ruey-Hsin,Huang Po-Hsun,Yin Wei-Hsian,Tseng Wei-Kung,Wu Yen-Wen,Lin Tsung-Hsien,Yeh Hung-I,Chang Kuan-Cheng,Wang Ji-Hung,Wu Chau-Chung,Chen Jaw-Wen

Abstract

Abstract Background Both the clinical and mechanistic impacts of endocan were not well elucidated especially in coronary artery disease (CAD). Objective This study aimed to investigate the prognostic and potential pathological role of endocan for cardiovascular (CV) events in stable CAD patients. Methods A total of 1,071 stable CAD patients with previous percutaneous coronary intervention (PCI) were enrolled prospectively in a nationwide Biosignature study. Another cohort of 76 CAD patients with or without PCI were enrolled for validation. Baseline biomarkers including endocan level was measured and total CV events especially hard CV events (including CV mortality, non-fatal myocardial infection and stroke) during follow-up were identified. Circulating endothelial progenitor cells (EPCs) as an in vivo biological contributor to vascular repairment from CAD patients were used for the in vitro functional study. Results After 24 months, there were 42 patients (3.92%) with hard CV events and 207 (19.3%) with total CV events in the study group. The incidence of both events was increased with the tertiles of baseline endocan level (hard events: 1.7%,3.4%, and 6.7% in 1st,2nd, and 3rd tertile respectively, p = 0.002; total events: 13.8%vs.16.2%vs.28.0%, p < 0.0001). Multivariate regression analysis revealed the independent association of endocan level with total and hard CV events. These findings were validated in another cohort with a 5-year follow-up. Furthermore, in vitro inhibition of endocan improved cell migration and tube formation capacities, and reduced cell adhesiveness of EPCs from CAD patients. Conclusions Endocan might be a novel prognostic indicator, mechanistic mediator, and potential therapeutic target for clinical CAD. Graphical abstract

Funder

Taipei Veterans General Hospital

National Science and Technology Council

Publisher

Springer Science and Business Media LLC

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