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用于慢性稳定型心绞痛管理的靶向心肌代谢的药物制剂:最新进展

Pharmacological Agents Targeting Myocardial Metabolism for the Management of Chronic Stable Angina : an Update.

作者信息

Guarini Giacinta, Huqi Alda, Morrone Doralisa, Marzilli Mario

机构信息

Cardiovascular Medicine Division, Cardio Thoracic and Vascular Department, University of Pisa, Via Paradisa n 2, 56100, Pisa, Italy.

出版信息

Cardiovasc Drugs Ther. 2016 Aug;30(4):379-391. doi: 10.1007/s10557-016-6677-y.

Abstract

Despite continuous advances in myocardial revascularization procedures and intracoronary devices, patients with ischemic heart disease (IHD) still experience worse prognosis and poor quality of life (QoL). Indeed, chronic stable angina (CSA) is a common disease with a large burden on healthcare costs. Traditionally, CSA is interpreted as episodes of reversible myocardial ischemia related to the presence of stable coronary artery plaque causing myocardial demand/supply mismatch when myocardial oxygen consumption increases. Accordingly, revascularization procedures are performed with the aim to remove the flow limiting stenosis, whereas traditional medical therapy (hemodynamic agents) aims at reducing myocardial oxygen demands. However, although effective, none of these treatment strategies or their combination is either able to confer symptomatic relief in all patients, nor to reduce mortality. Failure to significantly improve QoL and prognosis may be attributed at least in part to this "restrictive" understanding of IHD. Despite for many years myocardial metabolic derangement has been overlooked, recently it has gained increased attention with the development of new pharmacological agents (metabolic modulators) able to influence myocardial substrate selection and utilization thus improving cardiac efficiency. Shifting cardiac metabolism from free fatty acids (FA) towards glucose is a promising approach for the treatment of patients with stable angina, independently of the underling disease (macrovascular and/or microvascular disease). In this sense cardiac metabolic modulators open the way to a "revolutionary" understanding of ischemic heart disease and its common clinical manifestations, where myocardial ischemia is no longer considered as the mere oxygen and metabolites demand/supply unbalance, but as an energetic disorder. Keeping in mind such an alternative approach to the disease, development of new pharmacological agents directed toward multiple metabolic targets is mandatory.

摘要

尽管心肌血运重建手术和冠状动脉内装置不断取得进展,但缺血性心脏病(IHD)患者的预后仍然较差,生活质量(QoL)也很低。事实上,慢性稳定型心绞痛(CSA)是一种常见疾病,给医疗成本带来了巨大负担。传统上,CSA被解释为与稳定冠状动脉斑块的存在相关的可逆性心肌缺血发作,当心肌氧消耗增加时会导致心肌需求/供应不匹配。因此,进行血运重建手术的目的是消除血流限制性狭窄,而传统药物治疗(血流动力学药物)旨在降低心肌氧需求。然而,尽管这些治疗策略或其组合有效,但它们都无法使所有患者获得症状缓解,也无法降低死亡率。未能显著改善生活质量和预后至少部分可归因于对IHD的这种“限制性”理解。尽管多年来心肌代谢紊乱一直被忽视,但最近随着能够影响心肌底物选择和利用从而提高心脏效率的新型药物(代谢调节剂)的开发,它受到了越来越多的关注。将心脏代谢从游离脂肪酸(FA)转向葡萄糖是治疗稳定型心绞痛患者的一种有前景的方法,与潜在疾病(大血管和/或微血管疾病)无关。从这个意义上说,心脏代谢调节剂为对缺血性心脏病及其常见临床表现的“革命性”理解开辟了道路,在这种理解中,心肌缺血不再仅仅被视为氧和代谢物需求/供应失衡,而是一种能量紊乱。牢记这种针对该疾病的替代方法,开发针对多个代谢靶点的新型药物是必不可少的。

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