Reina-Couto Marta, Silva-Pereira Carolina, Pereira-Terra Patrícia, Quelhas-Santos Janete, Bessa João, Serrão Paula, Afonso Joana, Martins Sandra, Dias Cláudia Camila, Morato Manuela, Guimarães João T, Roncon-Albuquerque Roberto, Paiva José-Artur, Albino-Teixeira António, Sousa Teresa
Departamento de Biomedicina-Unidade de Farmacologia e Terapêutica, Faculdade de Medicina da Universidade do Porto (FMUP), Porto, Portugal.
Centro de Investigação Farmacológica e Inovação Medicamentosa, Universidade do Porto (MedInUP), Porto, Portugal.
Front Physiol. 2022 Aug 11;13:965611. doi: 10.3389/fphys.2022.965611. eCollection 2022.
Inflammation-driven endothelitis seems to be a hallmark of acute heart failure (AHF) and cardiogenic shock (CS). Endocan, a soluble proteoglycan secreted by the activated endothelium, contributes to inflammation and endothelial dysfunction, but has been scarcely explored in human AHF. We aimed to evaluate serum (S-Endocan) and urinary endocan (U-Endocan) profiles in AHF and CS patients and to correlate them with biomarkers/parameters of inflammation, endothelial activation, cardiovascular dysfunction and prognosis. Blood and spot urine were collected from patients with AHF ( = 23) or CS ( = 25) at days 1-2 (admission), 3-4 and 5-8 and from controls (blood donors, = 22) at a single time point. S-Endocan, U-Endocan, serum IL-1β, IL-6, tumour necrosis factor-α (S-TNF-α), intercellular adhesion molecule-1 (S-ICAM-1), vascular cell adhesion molecule-1 (S-VCAM-1) and E-selectin were determined by ELISA or multiplex immunoassays. Serum C-reactive protein (S-CRP), plasma B-type natriuretic peptide (P-BNP) and high-sensitivity troponin I (P-hs-trop I), lactate, urea, creatinine and urinary proteins, as well as prognostic scores (APACHE II, SAPS II) and echocardiographic left ventricular ejection fraction (LVEF) were also evaluated. Admission S-Endocan was higher in both patient groups, with CS presenting greater values than AHF (AHF and CS vs. Controls, < 0.001; CS . AHF, < 0.01). Admission U-Endocan was only higher in CS patients ( < 0.01 . Controls). At admission, S-VCAM-1, S-IL-6 and S-TNF-α were also higher in both patient groups but there were no differences in S-E-selectin and S-IL-1β among the groups, nor in P-BNP, S-CRP or renal function between AHF and CS. Neither endocan nor other endothelial and inflammatory markers were reduced during hospitalization ( > 0.05). S-Endocan positively correlated with S-VCAM-1, S-IL-6, S-CRP, APACHE II and SAPS II scores and was positively associated with P-BNP in multivariate analyses. Admission S-Endocan raised in line with LVEF impairment ( = 0.008 for linear trend). Admission endocan significantly increases across AHF spectrum. The lack of reduction in endothelial and inflammatory markers throughout hospitalization suggests a perpetuation of endothelial dysfunction and inflammation. S-Endocan appears to be a biomarker of endothelitis and a putative therapeutic target in AHF and CS, given its association with LVEF impairment and P-BNP and its positive correlation with prognostic scores.
炎症驱动的内皮炎似乎是急性心力衰竭(AHF)和心源性休克(CS)的一个标志。内脂素是一种由活化内皮细胞分泌的可溶性蛋白聚糖,它会导致炎症和内皮功能障碍,但在人类AHF中鲜有研究。我们旨在评估AHF和CS患者的血清(S-内脂素)和尿内脂素(U-内脂素)水平,并将它们与炎症、内皮激活、心血管功能障碍和预后的生物标志物/参数相关联。在第1 - 2天(入院时)、3 - 4天和5 - 8天从AHF患者(n = 23)或CS患者(n = 25)中采集血液和随机尿样,并在单一时间点从对照组(献血者,n = 22)中采集样本。通过酶联免疫吸附测定(ELISA)或多重免疫测定法测定S-内脂素、U-内脂素、血清白细胞介素-1β(IL-1β)、IL-6、肿瘤坏死因子-α(S-TNF-α)、细胞间黏附分子-1(S-ICAM-1)、血管细胞黏附分子-1(S-VCAM-1)和E-选择素。还评估了血清C反应蛋白(S-CRP)、血浆B型利钠肽(P-BNP)和高敏肌钙蛋白I(P-hs-trop I)、乳酸、尿素、肌酐和尿蛋白,以及预后评分(急性生理与慢性健康状况评分系统II [APACHE II]、简化急性生理学评分系统II [SAPS II])和超声心动图左心室射血分数(LVEF)。两组患者入院时的S-内脂素均较高,CS组的值高于AHF组(AHF组和CS组与对照组相比,P < 0.001;CS组与AHF组相比,P < 0.01)。入院时U-内脂素仅在CS患者中较高(P < 0.01与对照组相比)。入院时,两组患者的S-VCAM-1、S-IL-6和S-TNF-α也较高,但各组间S-E-选择素和S-IL-1β无差异,AHF组和CS组之间的P-BNP、S-CRP或肾功能也无差异。住院期间内脂素及其他内皮和炎症标志物均未降低(P > 0.05)。S-内脂素与S-VCAM-1、S-IL-6、S-CRP、APACHE II和SAPS II评分呈正相关,在多变量分析中与P-BNP呈正相关。入院时S-内脂素随LVEF损害而升高(线性趋势P = 0.008)。在整个AHF范围内,入院时内脂素显著升高。住院期间内皮和炎症标志物缺乏降低表明内皮功能障碍和炎症持续存在。鉴于S-内脂素与LVEF损害和P-BNP相关,且与预后评分呈正相关,它似乎是内皮炎的生物标志物以及AHF和CS中一个假定的治疗靶点。
