Tóth Štefan, Fedačko Ján, Pekárová Tímea, Hertelyová Zdenka, Katz Matan, Mughees Adil, Kuzma Jozef, Štefanič Peter, Kopolovets Ivan, Pella Daniel
1st Department of Internal Medicine, Faculty of Medicine, Pavol Jozef Safarik University, Trieda SNP 1, 041 90, Košice, Slovakia.
1st Department of Experimental Medicine, Faculty of Medicine, Pavol Jozef Safarik University, Trieda SNP 1, 041 90, Košice, Slovakia.
Cardiol Ther. 2017 Dec;6(2):281-289. doi: 10.1007/s40119-017-0092-8. Epub 2017 Jun 16.
Many studies have highlighted the important role of PCSK9 in the development of cardiometabolic changes and its possible function as a biomarker of myocardial infarction or ischemic heart disease. This study aimed to determine the relationship between circulating PCSK9 levels and subclinical vascular changes in the group of low risk patients without manifest cardiovascular diseases.
In this study, 120 healthy patients, free of manifest cardiovascular diseases, diabetes mellitus, and without lipid-lowering therapy, were divided into three groups based on BMI: normal weight (N = 50), overweight (N = 30), and obese (N = 40). Biochemical parameters, including basic lipid and non-lipid ones, were analyzed. PCSK9 levels were measured by ELISA, vascular changes were quantified by carotid ultrasound (carotid artery intima-media thickness, cIMT), and arterial stiffness parameters (pulse wave velocity, PWV; augmentation index, AI; stiffness parameter, β) were measured by an echo-tracking method.
Plasma levels of PCSK9 significantly increased in obese (172.78 ± 51.67 ng/mL) in comparison with overweight (120.14 ± 37.64, p < 0.001) and normal weight groups (114.92 ± 35.87, p < 0.001). Differences between the overweight and normal weight groups were not significant (p = 0.85). The level of PCSK9 significantly correlated with values of BMI (p < 0.001, r = 0.38). In addition to increase in laboratory parameters associated with moderate metabolic changes, significant increase in cIMT and parameters of vascular changes (β, AI, PWV) were detected in groups with elevated BMI. Significant positive linear correlation of PCSK9 concentrations and cIMT (p < 0.001, r = 0.39), PWV (p < 0.001, r = 0.31), and β (p < 0.001, r = 0.3) were found. In multivariable regression analysis after adjusting for gender, age, BMI, and LDL, the impact of PCSK9 on cIMT, β, and PWV remained significant (p = 0.006, 0.03, and 0.002, respectively).
PCSK9 plasma levels significantly correlated with subclinical vascular changes and their values were significantly elevated in obese subjects. We assume that PCSK9 could be used as a predictor of early vascular involvement, prior to the existence of manifest atherosclerosis. These results also highlight the role of anti-PCSK9 treatment in primary prevention.
许多研究强调了前蛋白转化酶枯草溶菌素9(PCSK9)在心脏代谢变化发展中的重要作用及其作为心肌梗死或缺血性心脏病生物标志物的潜在功能。本研究旨在确定无明显心血管疾病的低风险患者群体中循环PCSK9水平与亚临床血管变化之间的关系。
在本研究中,120名无明显心血管疾病、糖尿病且未接受降脂治疗的健康患者根据体重指数(BMI)分为三组:正常体重组(N = 50)、超重组(N = 30)和肥胖组(N = 40)。分析了包括基本脂质和非脂质参数在内的生化参数。通过酶联免疫吸附测定(ELISA)法测量PCSK9水平,通过颈动脉超声(颈动脉内膜中层厚度,cIMT)对血管变化进行量化,并通过回声跟踪法测量动脉僵硬度参数(脉搏波速度,PWV;增强指数,AI;僵硬度参数,β)。
与超重组(120.14±37.64,p < 0.001)和正常体重组(114.92±35.87,p < 0.001)相比,肥胖组(172.78±51.67 ng/mL)的血浆PCSK9水平显著升高。超重组与正常体重组之间的差异不显著(p = 0.85)。PCSK9水平与BMI值显著相关(p < 0.001,r = 0.38)。除了与中度代谢变化相关的实验室参数增加外,在BMI升高的组中还检测到cIMT和血管变化参数(β、AI、PWV)显著增加。发现PCSK9浓度与cIMT(p < 0.001,r = 0.39)、PWV(p < 0.001,r = 0.31)和β(p < 0.001,r = 0.3)之间存在显著的正线性相关。在对性别、年龄、BMI和低密度脂蛋白(LDL)进行校正后的多变量回归分析中,PCSK9对cIMT、β和PWV的影响仍然显著(分别为p = 0.006、0.03和0.002)。
血浆PCSK9水平与亚临床血管变化显著相关,且在肥胖受试者中其值显著升高。我们认为PCSK9可作为早期血管受累的预测指标,早于明显动脉粥样硬化的出现。这些结果也凸显了抗PCSK9治疗在一级预防中的作用。
