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Aortic valve disease in diabetes: Molecular mechanisms and novel therapies

机译:糖尿病中的主动脉瓣病:分子机制和新的疗法

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Valve disease and particularly calcific aortic valve disease (CAVD) and diabetes (DM) are progressive diseases constituting a global health burden for all aging societies ( Progress in Cardiovascular Diseases . 2014;56(6):565: Circulation Research . 2021;128(9):1344). Compared to non-diabetic individuals ( The Lancet . 2008;371(9626):1800: The American Journal of Cardiology . 1983;51(3):403: Journal of the American College of Cardiology . 2017;69(12):1523), the diabetic patients have a significantly greater propensity for cardiovascular disorders and faster degeneration of implanted bioprosthetic aortic valves. Previously, using an original experimental model, the diabetic-hyperlipemic hamsters, we have shown that the earliest alterations induced by these conditions occur at the level of the aortic valves and, with time these changes lead to calcifications and CAVD. However, there are no pharmacological treatments available to reverse or retard the progression of aortic valve disease in diabetes, despite the significant advances in the field. Therefore, it is critical to uncover the mechanisms of valve disease progression, find biomarkers for diagnosis and new targets for therapies. This review aims at presenting an update on the basic research in CAVD in the context of diabetes. We provide an insight into the accumulated data including our results on diabetes-induced progressive cell and molecular alterations in the aortic valve, new potential biomarkers to assess the evolution and therapy of the disease, advancement in targeted nanotherapies, tissue engineering and the potential use of circulating endothelial progenitor cells in CAVD.
机译:瓣膜疾病和特别是钙化主动脉瓣病(CAVD)和糖尿病(DM)是所有老化社会的全球健康负担的渐进疾病(心血管疾病的进展。2014; 56(6):565:流通研究。2021; 128( 9):1344)。与非糖尿病个体(柳叶刀)相比(2008年; 371(9626):1800:美国心脏病学杂志。1983; 51(3):403:美国心脏病学院学报。2017; 69(12):1523 ),糖尿病患者对心血管疾病的显着提高倾向,植入的生物假体主动脉瓣膜的变化更快。以前,使用原始实验模型,糖尿病高脂肪虫仓鼠,我们已经表明,这些条件的最早改变发生在主动脉瓣的水平,并且随着时间的变化导致钙化和CAVD。然而,尽管该领域的显着进展,但没有可用于逆转或延迟主动脉瓣病的进展的药理治疗。因此,揭示瓣膜疾病进展的机制至关重要,找到诊断和新疗法的生物标志物。该审查旨在提出糖尿病背景下的CAVD基础研究的更新。我们对累积数据提供了洞察,包括我们的糖尿病诱导的渐进细胞和主动脉瓣中的分子改变,新的潜在生物标志物评估疾病的演化和治疗,有针对性的纳米疗法,组织工程和潜在使用的进步脉冲中的循环内皮祖细胞。

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