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中国患者首次 PCI 后再次血运重建的血小板反应性及临床结局的 NOS3、MMP3、AGT 和 AGT1R 候选基因及通路分析

Candidate Gene of NOS3, MMP3, AGT, and AGT1R and Pathway Analyses for Platelet Reactivity and Clinical Outcomes of Repeat Revascularization After First PCI in Chinese Patients.

机构信息

Department of Pharmacy, Peking University First Hospital, No. 6, Da Hong Luo Chang Street, Xicheng District, Beijing, 100034, China.

Department of Cardiology, Peking University First Hospital, No. 8, Xi Shi Ku Da Street, Xicheng District, Beijing, 100034, China.

出版信息

Cardiovasc Drugs Ther. 2023 Jun;37(3):507-518. doi: 10.1007/s10557-021-07281-0. Epub 2021 Dec 3.

Abstract

PURPOSE

Major disadvantages of the percutaneous coronary intervention (PCI) are the high occurrence of repeat revascularization due to restenosis and disease progression. The current study aimed to identify indicators that can predict the risk of repeat revascularization.

METHODS

A total of 143 patients who underwent PCI and had genetic test results were enrolled. We retrospectively reviewed their medical records after the first PCI. P2Y12 reaction unit (PRU) test results were obtained by VerifyNow; 4 candidate genes (NOS3, MMP3, AGT, and AGT1R) and 380 genes related to platelet activation-related processes and clopidogrel activity were selected for analysis. Repeat revascularization and in-stent restenosis (ISR) were used as clinical outcomes, and PRU and ADP aggregation rates were used as platelet function outcomes in analysis.

RESULTS

After the first PCI, the incidence of repeat revascularization at 18, 30, and 42 months was 14.1% (20/142), 17.5% (24/137), and 39.7% (31/78), respectively. In the candidate gene analysis, rs7830 (NOS3) was associated with both ADP aggregation rate and 18- and 30-month ISR, and rs 62,275,847 (AGTR1) was associated with both ADP aggregation rate and 30-month ISR. In the pathway, gene-set analysis, the linkage rs471683 and rs7785386 of GNAI1|GNAT3 were associated with PRU and ADP aggregation rate, 18-month and 30-month ISR, and repeat revascularization within 30 months. Rs1715389 of GNAI1|GNAT3 was associated with both PRU and ADP aggregation rate, 18-month and 30-month ISR, and repeat revascularization within 30 months. Rs7313458 of ITPR2 was associated with PRU and ADP aggregation rate, 18-month and 30-month ISR, and repeat revascularization within 18 months.

CONCLUSIONS

The genetic polymorphisms of rs7830 (NOS3), rs62275874 (AGTR1), linkage rs471683 and rs7785386 (GNAI1|GNAT3), rs1715389 (GNAI1|GNAT3), and rs7313458 (ITPR2) may lead to an increased risk of in-stent restenosis and revascularization after the first PCI in Chinese patients by affecting the efficacy of clopidogrel. The above six SNP may be used as potential genetic biomarkers for high risk of in-stent restenosis and revascularization after the first PCI in Chinese patients.

摘要

目的

经皮冠状动脉介入治疗(PCI)的主要缺点是由于再狭窄和疾病进展导致再次血运重建的发生率较高。本研究旨在确定可预测再次血运重建风险的指标。

方法

共纳入 143 例接受 PCI 且有基因检测结果的患者。我们回顾性分析了他们首次 PCI 后的病历。通过 VerifyNow 获得 P2Y12 反应单位(PRU)检测结果;选择 4 个候选基因(NOS3、MMP3、AGT 和 AGT1R)和 380 个与血小板激活相关过程和氯吡格雷活性相关的基因进行分析。将重复血运重建和支架内再狭窄(ISR)作为临床结果,将 PRU 和 ADP 聚集率作为血小板功能结果进行分析。

结果

首次 PCI 后 18、30 和 42 个月的重复血运重建发生率分别为 14.1%(20/142)、17.5%(24/137)和 39.7%(31/78)。在候选基因分析中,rs7830(NOS3)与 ADP 聚集率和 18 个月和 30 个月 ISR 相关,rs62275874(AGTR1)与 ADP 聚集率和 30 个月 ISR 相关。在通路、基因集分析中,GNAI1|GNAT3 的连锁 rs471683 和 rs7785386 与 PRU 和 ADP 聚集率、18 个月和 30 个月 ISR 以及 30 个月内的重复血运重建相关。GNAI1|GNAT3 的 rs1715389 与 PRU 和 ADP 聚集率、18 个月和 30 个月 ISR 以及 30 个月内的重复血运重建相关。ITPR2 的 rs7313458 与 PRU 和 ADP 聚集率、18 个月和 30 个月 ISR 以及 18 个月内的重复血运重建相关。

结论

rs7830(NOS3)、rs62275874(AGTR1)、连锁 rs471683 和 rs7785386(GNAI1|GNAT3)、rs1715389(GNAI1|GNAT3)和 rs7313458(ITPR2)的遗传多态性可能通过影响氯吡格雷的疗效,导致中国患者首次 PCI 后支架内再狭窄和血运重建的风险增加。上述六个 SNP 可能成为中国患者首次 PCI 后支架内再狭窄和血运重建高危的潜在遗传生物标志物。

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