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配对风险评分预测急性冠状动脉综合征后 28 天至 1 年的缺血和出血风险。

Paired risk scores to predict ischaemic and bleeding risk twenty-eight days to one year after an acute coronary syndrome.

机构信息

Department of Medicine, The University of Auckland, Auckland, New Zealand

Cardiology Department, Middlemore Hospital, Auckland, New Zealand.

出版信息

Heart. 2023 Nov 27;109(24):1827-1836. doi: 10.1136/heartjnl-2023-322830.

Abstract

OBJECTIVE

The recommended duration of dual anti-platelet therapy (DAPT) following acute coronary syndrome (ACS) varies from 1 month to 1 year depending on the balance of risks of ischaemia and major bleeding. We designed paired ischaemic and major bleeding risk scores to inform this decision.

METHODS

New Zealand (NZ) patients with ACS investigated with coronary angiography are recorded in the All NZ ACS Quality Improvement registry and linked to national health datasets. Patients were aged 18-84 years (2012-2020), event free at 28 days postdischarge and without atrial fibrillation. Two 28-day to 1-year postdischarge multivariable risk prediction scores were developed: (1) cardiovascular mortality/rehospitalisation with myocardial infarction or ischaemic stroke (ischaemic score) and (2) bleeding mortality/rehospitalisation with bleeding (bleeding score).

FINDINGS

In 27 755 patients, there were 1200 (4.3%) ischaemic and 548 (2.0%) major bleeding events. Both scores were well calibrated with moderate discrimination performance (Harrell's c-statistic 0.75 (95% CI, 0.74 to 0.77) and 0.69 (95% CI, 0.67 to 0 .71), respectively). Applying these scores to the 2020 European Society of Cardiology ACS antithrombotic treatment algorithm, the 31% of the cohort at elevated (>2%) bleeding and ischaemic risk would be considered for an abbreviated DAPT duration. For those at low bleeding risk, but elevated ischaemic risk (37% of the cohort), prolonged DAPT may be appropriate, and for those with low bleeding and ischaemic risk (29% of the cohort) short duration DAPT may be justified.

CONCLUSION

We present a pair of ischaemic and bleeding risk scores specifically to assist clinicians and their patients in deciding on DAPT duration beyond the first month post-ACS.

摘要

目的

根据缺血和大出血风险的平衡,急性冠脉综合征(ACS)后双联抗血小板治疗(DAPT)的推荐持续时间从 1 个月到 1 年不等。我们设计了配对的缺血和大出血风险评分来辅助决策。

方法

新西兰(NZ)接受冠状动脉造影检查的 ACS 患者在全 NZ ACS 质量改进登记处进行登记,并与国家健康数据集相链接。患者年龄为 18-84 岁(2012-2020 年),出院后 28 天内无事件且无房颤。我们开发了两种出院后 28 天至 1 年的多变量风险预测评分:(1)心血管死亡率/再入院伴心肌梗死或缺血性卒中和(缺血评分)和(2)出血死亡率/再入院伴出血(出血评分)。

结果

在 27755 例患者中,有 1200 例(4.3%)发生缺血事件和 548 例(2.0%)发生大出血事件。这两个评分均具有良好的校准度和中等的区分度(Harrell's c 统计量分别为 0.75(95%CI,0.74 至 0.77)和 0.69(95%CI,0.67 至 0.71))。将这些评分应用于 2020 年欧洲心脏病学会 ACS 抗栓治疗算法,2020 年欧洲心脏病学会 ACS 抗栓治疗算法中,31%的患者出血和缺血风险升高(>2%),可能需要缩短 DAPT 持续时间。对于那些出血风险低但缺血风险升高(队列的 37%)的患者,可能需要延长 DAPT,而对于那些出血和缺血风险均低(队列的 29%)的患者,DAPT 持续时间较短可能是合理的。

结论

我们提出了一对缺血和出血风险评分,专门用于协助临床医生及其患者在 ACS 后第一个月之后决定 DAPT 的持续时间。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7286/10715548/287fe2db776a/heartjnl-2023-322830f01.jpg

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