The pharmacology of cholesterol-lowering drugs: The pharmacology of cholesterol-lowering drugs

European Atherosclerosis Journal Pub Date : 2022-04-05 DOI:10.56095/eaj.v1i1.7

C. Ballantyne, A. Catapano

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Abstract

The causal role of low-density lipoprotein cholesterol LDL-C in atherosclerotic-related cardiovascular disease (ASCVD) has been undoubtedly established over the last decades, and lowering plasma LDL-C levels represents the main approach to reduce the risk of cardiovascular (CV) events. A large number of observations has definitely proven that the protective effect is independent of the drug used to lower LDL-C, with a continuous linear reduction of CV risk with further LDL-C reductions. Although high-intensity statin therapy may significantly reduce CV event incidence, frequently statins are insufficient to achieve the large reductions recommended by current guidelines for high and very high risk patients. Several non-statin drugs, having mechanisms of action complementary to that of statins, are now available, and include ezetimibe, monoclonal antibodies targeting PCSK9, and, more recently, inclisiran, bempedoic acid, and evinacumab. Combining these drugs based on the recommendations by current and future guidelines should be considered for optimal risk reduction, although several gaps in clinical practice remain to be filled.

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降胆固醇药物的药理学降胆固醇药物的药理学

在过去的几十年中，低密度脂蛋白胆固醇LDL-C在动脉粥样硬化相关心血管疾病(ASCVD)中的因果作用已经毋庸置疑地确立，降低血浆LDL-C水平是降低心血管(CV)事件风险的主要途径。大量的观察已经明确证明，这种保护作用与用于降低LDL-C的药物无关，随着LDL-C的进一步降低，心血管风险呈持续的线性降低。尽管高强度他汀类药物治疗可以显著降低心血管事件的发生率，但他汀类药物通常不足以实现当前指南对高危和极高危患者推荐的大幅降低发生率。现在有几种非他汀类药物，具有与他汀类药物互补的作用机制，包括依折替米、靶向PCSK9的单克隆抗体，以及最近的inclisiran、苯足酸和evinacumab。应考虑根据当前和未来指南的建议联合使用这些药物，以最佳地降低风险，尽管临床实践中的一些空白仍有待填补。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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European Atherosclerosis Journal

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