Fibrotic changes in patients with chronic heart failure with cardiac dyssynchrony and associated type 2 diabetes mellitus

T. Rudenko, O. M. Khvysiuk, O. Godlevska, A. P. Braslavska
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Abstract

The study of fibrosis markers was carried out on 72 observed patients (mean age (69 ± 10.37) years) with chronic heart failure (CHF) of ischemic genesis with manifestations of cardiac dyssynchrony (CD) and concomitant type 2 diabetes mellitus – Galectin 3 and matrix metalloproteinase 1. All patients were divided into 2 groups, depending on the presence of CD. The CD was evaluated according to a conventional technique, the volume fraction of interstitial collagen was measured using the formula of J. Shirani and co-authors, the levels of Galectin-3 and matrix metalloproteinase 1 – by the enzyme-linked immunoassay according to the manufacturer's instructions. The data were processed using parametric and nonparametric statistics. It was revealed that the level of fibrosis development was higher in the group of patients with CD than in the group without CD. This indicates the dependence of the development of myocardial sites asynchronous reduction with the presence of interstitial collagen development. That further requires the study of the effect of anti-fibrotic, anti-ischemic and hypoglycemic agents on the progression of CD to prevent subsequent myocardial remodeling.
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慢性心力衰竭合并心脏非同步化及相关2型糖尿病患者的纤维化改变
对72例伴有心脏非同步化(CD)表现的缺血性慢性心力衰竭(CHF)合并2型糖尿病患者(平均年龄(69±10.37)岁)进行了纤维化标志物研究——凝集素3和基质金属蛋白酶1。根据是否存在CD,将所有患者分为两组。CD根据常规技术进行评估,间质胶原的体积分数使用J. Shirani及其合作者的公式进行测量,半乳糖凝集素-3和基质金属蛋白酶1 -的水平通过酶联免疫分析法根据制造商的说明。使用参数统计和非参数统计对数据进行处理。结果显示,与非CD组相比,CD组的纤维化发展水平更高。这表明心肌位点的发展依赖于间质胶原的存在。这就需要进一步研究抗纤维化、抗缺血和降糖药物对CD进展的影响,以防止随后的心肌重构。
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