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Living the PCSK9 Adventure: from the Identification of a New Gene in Familial Hypercholesterolemia Towards a Potential New Class of Anticholesterol Drugs

机译:经历PCSK9历险记:从家族性高胆固醇血症新基因的鉴定到潜在的新型抗胆固醇药物

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A decade after our discovery of the involvement of proprotein convertase subtilisin/kexin type 9 (PCSK9) in cholesterol metabolism through the identification of the first mutations leading to hypercholesterolemia, PCSK9 has become one of the most promising targets in cholesterol and cardiovascular diseases. This challenging work in the genetics of hypercholesterolemia paved the way for a plethora of studies around the world allowing the characterization of PCSK9, its expression, its impact on reducing the abundance of LDL receptor, and the identification of loss-of-function mutations in hypocholesterolemia. We highlight the different steps of this adventure and review the published clinical trials especially those with the anti-PCSK9 antibodies evolocumab (AMG 145) and alirocumab (SAR236553/REGN727), which are in phase III trials. The promising results in lowering LDL cholesterol levels raise hope that the PCSK9 adventure will lead, after the large and long-term ongoing phase III studies evaluating efficacy and safety, to a new anticholesterol pharmacological class.
机译:通过确定导致高胆固醇血症的第一个突变,我们发现前蛋白转化酶枯草杆菌蛋白酶/ kexin型9(PCSK9)参与胆固醇代谢十年后,PCSK9已成为胆固醇和心血管疾病最有希望的靶标之一。高胆固醇血症的遗传学这一具有挑战性的工作为世界范围内的大量研究铺平了道路,从而使PCSK9的特性,其表达,其对降低LDL受体丰度的影响以及低胆固醇血症的功能丧失突变的鉴定成为可能。我们重点介绍了这一冒险过程的不同步骤,并回顾了已发表的临床试验,尤其是那些具有三阶段试验的抗PCSK9抗体evolocumab(AMG 145)和alirocumab(SAR236553 / REGN727)的临床试验。降低LDL胆固醇水平的有希望的结果使人们希望,在进行了长期,长期的评估疗效和安全性的III期临床研究之后,PCSK9将会引领一个新的抗胆固醇药理学类别。

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