Early and Short-term Use of PCSK9-Inhibitors on Coronary Plaque Stability in Acute Coronary Syndrome

Hiroki Uehara, T. Kajiya, Masami Abe, M. Nakata, Shingo Hosogi, Shinichiro Ueda
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Abstract

Proprotein convertase anti-subtilisin-kexin type 9 inhibitors (PCSK9Is) improve plaque volume and composition and reduce major adverse coronary events in chronic coronary artery disease. We evaluated the effects of the short-term use of PCSK9Is on coronary plaque stability in patients with acute coronary syndrome (ACS) using optical coherence tomography (OCT). This multicenter, open label randomized controlled trial. Enrolled 80 subjects met the inclusion criteria. Of these, 52 patients (age 60±11 years, 38 men, 14 women) with ST-elevated ACS who had undergone successful primary percutaneous coronary intervention with low-density lipoprotein cholesterol (LDL-C) levels >70 mg/dL while receiving high-intensity statins. Participants were randomly assigned to the PCSK9Is group (evolocumab 420 mg for 3 months, N=29) or the standard of care (SoC) group(N=23). OCT was performed at baseline (BL) and 3-months (3M) and 9- months (9M) after randomization to assess lipid-rich plaques in non-culprit lesions.The change in the minimum fibrous cap thickness (MFCT) from baseline to 9M was the primary endpoint. The percentage change in LDL-C levels from BL to 3M were significantly greater in the PCSK9Is group (-67.8±21.5% in the PCSK9Is group vs. -16.3±21.8% in the SoC group; p<0.0001) and though, the difference between two groups were disappeared from BL to 9M (-20.0±37.8% in the PCSK9Is group vs. -6.7±34.2% in the SoC group; p=0.20).The changes in MFCT from baseline to 9M were significantly greater in the PCSK9Is group, even after PCSK9Is discontinuation (100 μm [Interquartile range (IQR): 45–180 μm] vs. 50 μm [IQR: 0–110 μm]; p=0.032). Combination treatment with PCSK9Is and statins resulted in more marked plaque stabilization after ACS than SoC alone, and this effect persisted for 6 months after PCSK9I discontinuation. Adage-Joto study, UMIN ID No. 26516
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早期和短期使用 PCSK9 抑制剂对急性冠状动脉综合征冠状动脉斑块稳定性的影响
Proprotein convertase anti-subtilisin-kexin type 9 inhibitors (PCSK9Is)能改善斑块的体积和组成,减少慢性冠状动脉疾病的主要不良冠状动脉事件。 我们使用光学相干断层扫描(OCT)评估了短期使用 PCSK9Is 对急性冠状动脉综合征(ACS)患者冠状动脉斑块稳定性的影响。 这项多中心、开放标签随机对照试验。共有 80 名受试者符合纳入标准。其中,52 名患者(年龄为 60±11 岁,38 名男性,14 名女性)患有 ST 段抬高的急性冠状动脉综合征,曾成功接受初级经皮冠状动脉介入治疗,低密度脂蛋白胆固醇(LDL-C)水平大于 70 mg/dL,同时正在接受高强度他汀类药物治疗。参与者被随机分配到 PCSK9Is 组(evolocumab 420 毫克,3 个月,N=29)或标准护理(SoC)组(N=23)。基线(BL)、随机分组后3个月(3M)和9个月(9M)时进行OCT检查,以评估非病灶中富含脂质的斑块。 PCSK9Is组的LDL-C水平从基线到3M的百分比变化明显大于SoC组(PCSK9Is组为-67.8±21.5%,SoC组为-16.3±21.8%,P<0.0001),尽管从基线到9M两组间的差异消失了(PCSK9Is组为-20.0±37.8%,SoC组为-16.3±21.8%,P<0.0001)。PCSK9Is组从基线到9M的MFCT变化明显大于PCSK9Is组,即使在停用PCSK9Is后也是如此(100 μm [四分位间范围(IQR):45-180 μm] vs. 50 μm [四分位间范围(IQR):0-110 μm];P=0.032)。 与单独使用他汀类药物相比,PCSK9Is 和他汀类药物联合治疗可使 ACS 后的斑块趋于稳定,而且这种效果在 PCSK9I 停药后的 6 个月内持续存在。 Adage-Joto 研究,UMIN ID 编号:26516
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