胆固醇酯转移蛋白抑制的安全性和有效性：从遗传学到结果试验

IF 5.9 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS

American journal of preventive cardiology Pub Date : 2025-09-01 DOI:10.1016/j.ajpc.2025.101135

John JP Kastelein MD, PhD , Brian A. Ference MD, Mphil, FMedSci , Adam J Nelson MBBS, PhD , Stephen Nicholls MBBS, PhD , Kausik K Ray MD, Mphil, FMedSci

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引用次数: 0

摘要

研究背景：探讨HDL-C水平与死亡率和心血管（CV）事件之间的关系；CETP抑制导致HDL-C升高的安全性；以及CETP作为血脂改变治疗靶点的疗效。方法：使用工具变量遗传评分，比较英国生物银行（n ~ 44.5万）参与者的主要冠状动脉事件、CV死亡率和非CV死亡率的累积率，这些参与者按自然性质随机分配到不同水平的终生暴露于HDL-C（孟德尔随机化[MR]）。在英国生物银行（UK Biobank）或CARDloGRAMplusC4D联盟（n=630,070）的参与者中，按性质随机分配到CETP、HMG CoA还原酶和PCSK9抑制的参与者中，主要冠状动脉事件的累积率与载脂蛋白ob的绝对减少相同。采用调整治疗幅度和持续时间的随机对照试验的荟萃分析来估计CETP抑制引起的血浆HDL-C变化与全因和CV死亡风险之间的关系（n=58,412）；以及CETP抑制与主要CV事件、CV死亡率和全因死亡率之间的关系（n=42,541）。结果：观察性研究、MR研究或随机对照试验没有令人信服的明确证据表明，非常高的血浆HDL-C水平会增加全因、非CV或CV死亡的风险。CETP抑制与全因死亡率和CV死亡率的适度降低相关。MR和随机对照试验的随机证据一致表明，CETP抑制降低主要CV事件的风险与实现的血浆载脂蛋白降低成正比，并且与他汀类药物和PCSK9抑制剂实现的相同的载脂蛋白降低量大致相同。结论：CETP抑制导致的自然发生的HDL-C升高或治疗性HDL-C升高均与全因、CV或非CV死亡率升高无关。CETP抑制诱导的ApoB降低与他汀类药物和PCSK9抑制剂诱导的降低程度大致相同。

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SAFETY AND EFFICACY OF CHOLESTERYL ESTER TRANSFER PROTEIN INHIBITION: FROM GENETICS TO OUTCOME TRIALS

Therapeutic Area

ASCVD/CVD Risk Assessment

Background

To investigate the associations between HDL-C levels with mortality and cardiovascular (CV) events; the safety of increased HDL-C due to CETP inhibition; and the efficacy of CETP as a target of lipid-altering therapy.

Methods

The cumulative rates of major coronary events, CV mortality, and non-CV mortality were compared among participants in the UK Biobank (n∼445,000) who were randomized by nature to different levels of lifetime exposure to HDL-C (Mendelian randomization [MR]) using an instrumental variable genetic score. The cumulative rates of major coronary events among participants randomized by nature to CETP, HMG CoA reductase, and PCSK9 inhibition was compared for the same absolute reduction in apoB among participants in the UK Biobank or CARDloGRAMplusC4D consortium (n=630,070). A Meta-analysis of RCTs adjusted for magnitude and duration of therapy was used to estimate the association between CETP inhibition induced changes in plasma HDL-C and the risk of both all-cause and CV mortality (n=58,412); and between CETP inhibition and the risk of major CV events, CV mortality, and all-cause mortality (n=42,541).

Results

There was no compelling unconfounded evidence from observational studies, MR studies, or RCTs that very high plasma HDL-C levels increase risk of all-cause, non-CV, or CV mortality. CETP inhibition is associated with a modestly lower risk of all-cause and CV mortality. There was consistent randomized evidence from MR and RCTs that CETP inhibition reduces risk of major CV events proportional to the achieved reduction in plasma apoB, and by approximately the same amount as statins and PCSK9 inhibitors for the same achieved reduction in apoB.

Conclusions

Neither naturally occurring elevated HDL-C or therapeutically increased HDL-C due to CETP inhibition are associated with increased all-cause, CV, or non-CV mortality. ApoB reduction induced by CETP inhibition reduces CV risk by approximately the same degree as reductions induced by statins and PCSK9 inhibitors.

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来源期刊

American journal of preventive cardiology Cardiology and Cardiovascular Medicine

CiteScore

6.60

自引率

0.00%

发文量

审稿时长

76 days