Human Genetic Laboratory, Faculty of Medicine, University of Medicine and Pharmacy, 200349 Craiova, Romania.
Department of Cardiology, University of Medicine and Pharmacy, 200349 Craiova, Romania.
Int J Mol Sci. 2021 Sep 7;22(18):9688. doi: 10.3390/ijms22189688.
ApoE abnormality represents a well-known risk factor for cardiovascular diseases. Beyond its role in lipid metabolism, novel studies demonstrate a complex involvement of apoE in membrane homeostasis and signaling as well as in nuclear transcription. Due to the large spread of apoE isoforms in the human population, there is a need to understand the apoE's role in pathological processes. Our study aims to dissect the involvement of apoE in heart failure. We showed that apoE-deficient rats present multiple organ damages (kidney, liver, lung and spleen) besides the known predisposition for obesity and affected lipid metabolism (two-fold increase in tissular damages in liver and one-fold increase in kidney, lung and spleen). Heart tissue also showed significant morphological changes in apoE rats, mostly after a high-fat diet. Interestingly, the right ventricle of apoE rats fed a high-fat diet showed more damage and affected collagen content (~60% less total collagen content and double increase in collagen1/collagen3 ratio) compared with the left ventricle (no significant differences in total collagen content or collagen1/collagen3 ratio). In patients, we were able to find a correlation between the presence of ε4 allele and cardiomyopathy (χ = 10.244; = 0.001), but also with right ventricle dysfunction with decreased TAPSE (15.3 ± 2.63 mm in ε4-allele-presenting patients vs. 19.8 ± 3.58 mm if the ε4 allele is absent, < 0.0001*) and increased in systolic pulmonary artery pressure (50.44 ± 16.47 mmHg in ε4-allele-presenting patients vs. 40.68 ± 15.94 mmHg if the ε4 allele is absent, = 0.0019). Our results confirm that the presence of the ε4 allele is a lipid-metabolism-independent risk factor for heart failure. Moreover, we show for the first time that the presence of the ε4 allele is associated with right ventricle dysfunction, implying different regulatory mechanisms of fibroblasts and the extracellular matrix in both ventricles. This is essential to be considered and thoroughly investigated before the design of therapeutical strategies for patients with heart failure.
载脂蛋白 E 异常是心血管疾病的一个众所周知的危险因素。除了在脂质代谢中的作用外,新的研究还表明载脂蛋白 E 在膜稳态和信号转导以及核转录中具有复杂的作用。由于载脂蛋白 E 同种型在人类中的广泛分布,因此需要了解载脂蛋白 E 在病理过程中的作用。我们的研究旨在剖析载脂蛋白 E 在心力衰竭中的作用。我们发现,载脂蛋白 E 缺乏的大鼠除了已知的肥胖倾向和脂质代谢受影响(肝组织损伤增加两倍,肾、肺和脾组织损伤增加一倍)外,还存在多个器官损伤(肾、肝、肺和脾)。在高脂肪饮食喂养的载脂蛋白 E 大鼠中,心脏组织也表现出明显的形态变化。有趣的是,与左心室相比,高脂肪饮食喂养的载脂蛋白 E 大鼠的右心室损伤更严重,胶原含量也受到影响(总胶原含量减少 60%,胶原 1/胶原 3 比值增加一倍)。在患者中,我们发现 ε4 等位基因的存在与心肌病(χ=10.244;=0.001)之间存在相关性,也与右心室功能障碍导致 TAPSE 降低(ε 4 等位基因存在的患者为 15.3±2.63mm,ε 4 等位基因缺失的患者为 19.8±3.58mm,<0.0001*)和收缩期肺动脉压升高(ε 4 等位基因存在的患者为 50.44±16.47mmHg,ε 4 等位基因缺失的患者为 40.68±15.94mmHg,=0.0019)相关。我们的结果证实,ε4 等位基因的存在是心力衰竭的一个与脂质代谢无关的危险因素。此外,我们首次表明,ε4 等位基因的存在与右心室功能障碍有关,这意味着两个心室中的成纤维细胞和细胞外基质的调节机制不同。在为心力衰竭患者设计治疗策略之前,这一点至关重要,需要进行深入研究。
