Cziráki Attila, Lenkey Zsófia, Sulyok Endre, Szokodi István, Koller Akos
Medical School, Heart Institute, University of Pécs, Pécs, Hungary.
Szentágothai Research Centre, University of Pécs, Pécs, Hungary.
Front Pharmacol. 2020 Sep 29;11:569914. doi: 10.3389/fphar.2020.569914. eCollection 2020.
By 1980, it was thought that we already knew most of the major mechanisms regulating vascular tone. However, after the somewhat serendipity discovery that endothelium is involved in mediation of relaxation to acetylcholine, a whole new world opened up and we had to rewrite our concept regarding vascular function and its regulation (not to mention many other fields). The new player was an endothelium derived relaxing factor, which molecular constitution has been identified to be nitric oxide (NO). This review summarizes the major molecular steps concerning how NO is synthetized from L-arginine. Also, the fate of L-arginine is described the arginase and methylation pathways; both of them are affecting substantially the level and efficacy of NO. and effects of L-arginine are summarized and controversial clinical findings are discussed. On the basis of the use of methylated L-arginines, the vasomotor effects of endothelial NO released to agonists and increases in flow/wall shear stress (a major biological stimulus) is summarized. In this review the role of NO in the regulation of coronary vascular resistance, hence blood flow, is delineated and the somewhat questionable clinical use of NO donors is discussed. We made an attempt to summarize the biosynthesis, role, and molecular mechanisms of endogenously produced methylated L-arginine, asymmetric dimethylarginine (ADMA) in modulating vascular resistance, affecting the function of the heart. Additionally, the relationship between ADMA level and various cardiovascular diseases is described, such as atherosclerosis, coronary artery disease (CAD), ischemia/reperfusion injuries, and different types of coronary revascularization. A novel aspect of coronary vasomotor regulation is identified in which the pericardial fluid ADMA and endothelin play putative roles. Finally, some of the open possibilities for future research on L-arginine-NO-ADMA signaling are highlighted.
到1980年,人们认为我们已经了解了调节血管张力的大部分主要机制。然而,在偶然发现内皮参与乙酰胆碱介导的舒张作用后,一个全新的世界展现在我们面前,我们不得不重新审视我们关于血管功能及其调节的概念(更不用说许多其他领域了)。这个新角色是一种内皮衍生的舒张因子,其分子结构已被确定为一氧化氮(NO)。这篇综述总结了关于NO如何从L-精氨酸合成的主要分子步骤。此外,还描述了L-精氨酸的去向——精氨酸酶和甲基化途径;它们都极大地影响了NO的水平和功效。还总结了L-精氨酸的作用,并讨论了有争议的临床发现。基于甲基化L-精氨酸的使用,总结了内皮NO释放到激动剂以及血流/壁面剪应力增加(一种主要的生物刺激)时的血管运动效应。在这篇综述中,阐述了NO在调节冠状动脉阻力从而调节血流中的作用,并讨论了NO供体在临床上有些可疑的用途。我们试图总结内源性产生的甲基化L-精氨酸——不对称二甲基精氨酸(ADMA)在调节血管阻力、影响心脏功能方面的生物合成、作用和分子机制。此外,还描述了ADMA水平与各种心血管疾病之间的关系,如动脉粥样硬化、冠状动脉疾病(CAD)、缺血/再灌注损伤以及不同类型的冠状动脉血运重建。确定了冠状动脉血管运动调节的一个新方面,即心包液ADMA和内皮素在其中可能发挥作用。最后,强调了未来关于L-精氨酸-NO-ADMA信号通路研究的一些开放可能性。
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