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通过调节四氢生物蝶呤和一氧化氮,释放一氧化氮的他汀类药物对心血管疾病影响的最新进展。

Recent developments in the effects of nitric oxide-donating statins on cardiovascular disease through regulation of tetrahydrobiopterin and nitric oxide.

作者信息

Ma Sze, Ma Christopher Cheng-Hwa

机构信息

Hong Kong Baptist Hospital, Hong Kong; National University Ireland, Ireland; Royal College of Physicians of Ireland, Ireland.

NHS Dumfries & Galloway, GMC 7411692, United Kingdom; King's College London School of Medicine, United Kingdom.

出版信息

Vascul Pharmacol. 2014 Nov;63(2):63-70. doi: 10.1016/j.vph.2014.08.001. Epub 2014 Aug 17.

Abstract

Since the discovery of the importance of nitric oxide (NO) to the human body three decades ago, numerous laboratory and clinical studies have been done to explore its potential therapeutic actions on many organs. In the cardiovascular system, NO works as a volatile signaling molecule regulating the vascular permeability and vascular tone, preventing thrombosis and inflammation, as well as inhibiting the smooth muscle hyperplasia. Thus, NO is important in the prevention and treatment of cardiovascular disease. NO is synthesized by NO synthase (NOS) with tetrahydrobiopterin (BH4) as the crucial cofactor. Many studies have been done to form nitric oxide donors so as to deliver NO directly to the vessel walls. In addition, NO moieties have been incorporated into existing therapeutic agents to enhance the NO bioavailability, including statins. Statins are inhibitors of 3-hydroxy-3-methylglutaryl-coenzyme (HMG-CoA), the rate-limiting enzyme of the mevalonate pathway. By inhibiting this pathway, statins lower blood cholesterol and exert their pleiotropic effects through activity in reaction cascades, such as Rho/ROCK and Rac 1/NADPH oxidase pathways. Statins have also been observed to implement their non-lipid effects by promoting BH4 synthesis with increase of NO bioavailability. Furthermore, NO-donating statins in laboratory studies have demonstrated to produce better therapeutic effects than their parent's drugs. They offer better anti-inflammatory, anti-proliferative and antithrombotic actions on cardiovascular system. They also cause better revascularization in peripheral ischemia and produce greater enhancement in limb reperfusion and salvage. In addition, it has been shown that NO-donating statin caused less myotoxicity, the most common side effect related to treatment with statins. The initial studies have demonstrated the superior therapeutic effects of NO-donating statins while producing fewer side effects.

摘要

自从三十年前发现一氧化氮(NO)对人体的重要性以来,已经进行了大量的实验室和临床研究,以探索其对许多器官的潜在治疗作用。在心血管系统中,NO作为一种挥发性信号分子,调节血管通透性和血管张力,预防血栓形成和炎症,并抑制平滑肌增生。因此,NO在心血管疾病的预防和治疗中很重要。NO由一氧化氮合酶(NOS)以四氢生物蝶呤(BH4)作为关键辅因子合成。已经进行了许多研究来形成一氧化氮供体,以便将NO直接递送至血管壁。此外,NO部分已被纳入现有的治疗药物中以提高NO的生物利用度,包括他汀类药物。他汀类药物是3-羟基-3-甲基戊二酰辅酶A(HMG-CoA)的抑制剂,HMG-CoA是甲羟戊酸途径的限速酶。通过抑制该途径,他汀类药物降低血液胆固醇,并通过在反应级联中的活性发挥其多效性作用,例如Rho/ROCK和Rac 1/NADPH氧化酶途径。还观察到他汀类药物通过促进BH4合成并增加NO生物利用度来发挥其非脂质作用。此外,实验室研究中的供NO他汀类药物已证明比其母体药物产生更好的治疗效果。它们在心血管系统上具有更好的抗炎、抗增殖和抗血栓形成作用。它们还能在周围缺血中引起更好的血管再通,并在肢体再灌注和挽救中产生更大的改善。此外,已经表明供NO他汀类药物引起的肌毒性较小,肌毒性是与他汀类药物治疗相关的最常见副作用。初步研究表明,供NO他汀类药物具有卓越的治疗效果,同时产生的副作用较少。

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