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Intraplatelet L-Arginine-Nitric Oxide Metabolic Pathway: From Discovery to Clinical Implications in Prevention and Treatment of Cardiovascular Disorders

机译:肾内伸缩式L-精氨酸 - 一氧化氮代谢途径:从发现到预防和治疗心血管障碍的临床意义

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Despite the development of new drugs and other therapeutic strategies, cardiovascular disease (CVD) remains still the major cause of morbidity and mortality in the world population. A lot of research, performed mostly in the last three decades, revealed an important correlation between “classical” demographic and biochemical risk factors for CVD, (i.e., hypercholesterolemia, hyperhomocysteinemia, smoking, renal failure, aging, diabetes, and hypertension) with endothelial dysfunction associated directly with the nitric oxide deficiency. The discovery of nitric oxide and its recognition as an endothelial-derived relaxing factor was a breakthrough in understanding the pathophysiology and development of cardiovascular system disorders. The nitric oxide synthesis pathway and its regulation and association with cardiovascular risk factors were a common subject for research during the last decades. As nitric oxide synthase, especially its endothelial isoform, which plays a crucial role in the regulation of NO bioavailability, inhibiting its function results in the increase in the cardiovascular risk pattern. Among agents altering the production of nitric oxide, asymmetric dimethylarginine—the competitive inhibitor of NOS—appears to be the most important. In this review paper, we summarize the role of L-arginine-nitric oxide pathway in cardiovascular disorders with the focus on intraplatelet metabolism.
机译:尽管新药和其他治疗策略的发展,心血管疾病(CVD)仍然是世界人口中发病率和死亡率的主要原因。大多数研究主要在过去三十年中表现出了“古典”人口统计学和生物化学危险因素的重要相关性,(即高胆固醇血症,高胆囊肿,吸烟,肾功能衰竭,老化,糖尿病和高血压)具有内皮功能障碍直接与一氧化氮缺乏症相关。作为内皮衍生的缓解因子的一氧化氮的发现及其识别是了解心血管系统疾病的病理生理学和发育方面的突破。一氧化氮合成途径及其调节和与心血管危险因素的调节和关联是过去几十年中研究的共同主题。作为一氧化氮合酶,尤其是其内皮同种型,其在没有生物利用度的调节中起着至关重要的作用,抑制其功能导致心血管风险模式的增加。在改变一氧化氮的产生的试剂中,不对称二甲基碱 - 竞争抑制剂的NOS-似乎是最重要的。在本文中,我们总结了L-精氨酸一氧化氮途径在心血管障碍中的作用,重点是肾内植物代谢。

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