Ying Qidi, Chan Dick C, Watts Gerald F
School of Medicine, Faculty of Health and Medical Sciences, University of Western Australia, Perth, WA, Australia.
Lipid Disorders Clinic, Department of Cardiology and Internal Medicine, Royal Perth Hospital, Perth, WA, Australia.
Front Physiol. 2021 Feb 10;12:603910. doi: 10.3389/fphys.2021.603910. eCollection 2021.
Proprotein convertase subtilisin/kexin type 9 (PCSK9) is a convertase enzyme mostly produced by the liver. It is a key regulator of LDL metabolism because of its ability to enhance degradation of the LDL receptor. PCSK9 also regulates the metabolism of lipoprotein(a) [Lp(a)] and triglyceride-rich lipoproteins (TRLs). Its key role in modulating atherosclerotic cardiovascular disease (ASCVD) is supported by genetic studies and clinical outcome trials. Kinetic studies provide mechanistic insight into the role of PCSK9 in regulating the physiology and pathophysiology of plasma lipids and lipoproteins. Kinetic data have demonstrated that plasma PCSK9 concentration is inversely associated with the clearance of LDL in men. Gain-of-function mutations of PCSK9 markedly increase plasma LDL-cholesterol concentrations due to impaired LDL-apoB catabolism. Conversely, PCSK9 deficiency results in low LDL-cholesterol associated with enhanced LDL-apoB clearance. Inhibition of PCSK9 with monoclonal antibodies (such as evolocumab or alirocumab) lowers plasma LDL-cholesterol and apoB levels chiefly by upregulating the catabolism of LDL particles in healthy individuals. As monotherapy, PCSK9 inhibitor reduced Lp(a) concentrations by decreasing the production rate. However, as combination therapy, it reduced the plasma concentration of Lp(a) by increasing the fractional catabolism of Lp(a) particles. In statin-treated patients with high Lp(a), PCSK9 inhibition lowers plasma Lp(a) concentrations by accelerating the catabolism of Lp(a) particles. The effect of PCSK9 inhibition on TRL metabolism has been studied in healthy individuals and in patients with type 2 diabetes. These findings suggest that PCSK9 appears to play a less important role in TRL than LDL metabolism. Kinetic studies of PCSK9 inhibition therapy on lipoprotein metabolism in diverse high risk patient populations (such as familial hypercholesterolemia) and new therapeutic combination also merit further investigation.
前蛋白转化酶枯草溶菌素/kexin 9型(PCSK9)是一种主要由肝脏产生的转化酶。由于其能够增强低密度脂蛋白(LDL)受体的降解,它是LDL代谢的关键调节因子。PCSK9还调节脂蛋白(a)[Lp(a)]和富含甘油三酯的脂蛋白(TRL)的代谢。基因研究和临床结局试验支持了其在调节动脉粥样硬化性心血管疾病(ASCVD)中的关键作用。动力学研究为PCSK9在调节血浆脂质和脂蛋白的生理及病理生理过程中的作用提供了机制性见解。动力学数据表明,男性血浆PCSK9浓度与LDL清除率呈负相关。PCSK9的功能获得性突变由于LDL-载脂蛋白B(apoB)分解代谢受损而显著增加血浆LDL胆固醇浓度。相反,PCSK9缺乏导致LDL胆固醇水平降低,同时LDL-apoB清除增强。用单克隆抗体(如依洛尤单抗或阿利西尤单抗)抑制PCSK9主要通过上调健康个体中LDL颗粒的分解代谢来降低血浆LDL胆固醇和apoB水平。作为单一疗法,PCSK9抑制剂通过降低生成速率来降低Lp(a)浓度。然而,作为联合疗法,它通过增加Lp(a)颗粒的分数分解代谢来降低血浆Lp(a)浓度。在接受他汀类药物治疗且Lp(a)水平高的患者中,抑制PCSK9可通过加速Lp(a)颗粒的分解代谢来降低血浆Lp(a)浓度。在健康个体和2型糖尿病患者中研究了抑制PCSK9对TRL代谢的影响。这些发现表明,PCSK9在TRL代谢中似乎比在LDL代谢中发挥的作用更小。对不同高危患者群体(如家族性高胆固醇血症)中PCSK9抑制疗法对脂蛋白代谢的动力学研究以及新的治疗组合也值得进一步研究。
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