稳定型冠心病患者经皮冠状动脉内介入治疗术后使用β阻滞剂不能降低全因死亡及主要不良心血管事件风险

doi:10.12122/j.issn.1673-4254.2026.01.17

摘要/Abstract

摘要：

目的探究稳定型冠心病（SCAD）患者经皮冠状动脉内介入治疗（PCI）术后β阻滞剂使用与全因死亡及主要不良心血管事件（MACEs）风险之间关联性。方法基于Dryad数据库进行二次分析，根据PCI术后是否使用β阻滞剂分为对照组（n=149）和β阻滞剂组（n=55），组间比较患者临床与冠脉病变特征，采用倾向性评分方法比较两组间全因死亡、MACEs（包括心血管死亡、非致死性心梗和非致死性卒中）之间的差异。结果共纳入204名SCAD患者，年龄72.6±10.3岁，其中69.6%为男性，中位随访时间为783 d。累计死亡患者18例（8.8%），发生MACEs 19例（9.3%），其中心血管死亡6例（2.9%），非致死性心梗3例（1.5%）、非致死性卒中11例（5.4%）。β阻滞剂组累计死亡5例（9.1%），发生MACEs 4例（7.3%），其中心血管死亡、非致死性心梗及非致死性卒中分别为2例（3.6%）、0例（0%）和2例（3.6%）。Kaplan-Meier生存曲线显示PCI术后β阻滞剂使用与否和降低全因死亡率及MACEs发生率无关（8.7% vs 9.1%， log-rank P = 0.870； 10.1% vs 7.3%， log-rank P=0.510）。在调整年龄、性别、谷草转氨酶、估算肾小球滤过率、左室射血分数及房颤病史等混杂因素后，β阻滞剂使用与SCAD患者PCI术后的全因死亡和MACEs风险不相关（HR 0.81， 95% CI： 0.24~2.72； HR 0.62，95% CI：0.22~1.69）。此外，基于倾向性评分校正、匹配或IPTW逆概率加权等的探索均未发现两组间在全因死亡与MACEs之间存在显著差异（均P>0.05）。结论基于Dryad数据库二次分析得出，稳定型冠心病患者PCI术后常规使用β阻滞剂并未能降低全因死亡和MACEs的发生。

关键词: 稳定型冠心病, 经皮冠状动脉内介入治疗, β阻滞剂, 全因死亡, 心血管不良事件

Abstract:

Objective To explore the association between the use of β-blockers and the risks of all-cause mortality and major adverse cardiovascular events (MACEs) in patients with stable coronary artery disease (SCAD) after percutaneous coronary intervention (PCI). Methods We performed secondary analyses of the data of 55 SCAD patients receiving post-PCI β-blocker treatment and 149 patients without post-PCI β‑blockers (control group) from the Dryad database. The clinical and coronary artery disease characteristics of the patients were analyzed, and propensity score matching was used to compare all-cause mortality and MACEs (including cardiovascular death, non-fatal myocardial infarction and non-fatal stroke) between the two groups. Results The overall patients (69.6% were male) had a mean age of 72.6±10.3 years with a median follow-up time of 783 days. A total of 18 patients (8.8%) died, and MACEs occurred in 19 patients (9.3%), including cardiovascular death in 6 cases (2.9%), non-fatal myocardial infarction in 3 cases (1.5%) and non-fatal stroke in 11 cases (5.4%). In the β‑blocker group, deaths occurred in 5 cases (9.1%), and MACEs in 4 cases (7.3%), including 2 cases with cardiovascular death (3.6%) and 2 cases with non-fatal stroke (3.6%). Kaplan-Meier survival curve analysis showed that the use of β-blockers after PCI was not associated with a reduced all-cause mortality (8.7% vs 9.1%, log-rank P=0.870) or incidence of MACEs (10.1% vs 7.3%, log-rank P=0.510) either before or after adjusting for age, sex, aspartate aminotransferase, estimated glomerular filtration rate, left ventricular ejection fraction, and history of atrial fibrillation (HR=0.81, 95% CI: 0.24-2.72; HR=0.62, 95% CI: 0.22-1.69). No significant differences were found in all-cause death or MACEs between the two groups after propensity score adjustment, matching, or IPTW inverse probability weighting (all P>0.05). Conclusion Routine use of β-blockers after PCI does not reduce the incidence of all-cause death or MACEs in patients with SCAD.

Key words: stable coronary artery disease, percutaneous coronary intervention, β-blockers, all-cause mortality, major adverse cardiovascular events

高希羽, 肖静, 冯娜, 郭晨, 曹丽菲, 张春艳, 张岩, 韩拓. 稳定型冠心病患者经皮冠状动脉内介入治疗术后使用β阻滞剂不能降低全因死亡及主要不良心血管事件风险[J]. 南方医科大学学报, 2026, 46(1): 159-165.

Xiyu GAO, Jing XIAO, Na FENG, Chen GUO, Lifei CAO, Chunyan ZHANG, Yan ZHANG, Tuo HAN. β‑blockers after percutaneous coronary intervention does not reduce risks of all-cause mortality or major adverse cardiovascular events in patients with stable coronary artery disease[J]. Journal of Southern Medical University, 2026, 46(1): 159-165.

图/表 4

参考文献 31

[1]	Chong B, Jayabaskaran J, Jauhari SM, et al. Global burden of cardiovascular diseases: projections from 2025 to 2050[J]. Eur J Prev Cardiol, 2025, 32(11): 1001-15. doi：10.1093/eurjpc/zwae281
[2]	中国心血管健康与疾病报告2024概要 [J]. 中国循环杂志, 2025, 40 (6): 521-59.
[3]	Navarese EP, Lansky AJ, Kereiakes DJ, et al. Cardiac mortality in patients randomised to elective coronary revascularisation plus medical therapy or medical therapy alone: a systematic review and meta-analysis[J]. Eur Heart J, 2021, 42(45): 4638-51. doi：10.1093/eurheartj/ehab246
[4]	Hahn JY, Song YB, Oh JH, et al. Effect of P2Y12 inhibitor monotherapy vs dual antiplatelet therapy on cardiovascular events in patients undergoing percutaneous coronary intervention: the SMART-CHOICE randomized clinical trial[J]. JAMA, 2019, 321(24): 2428-37. doi：10.1001/jama.2019.8146
[5]	Boberg J, Larsen FF, Pehrsson SK. The effects of beta blockade with (epanolol) and without (atenolol) intrinsic sympathomimetic activity in stable angina pectoris. The Visacor Study Group[J]. Clin Cardiol, 1992, 15(8): 591-5. doi：10.1002/clc.4960150808
[6]	Vantrimpont P, Rouleau JL, Wun CC, et al. Additive beneficial effects of beta-blockers to angiotensin-converting enzyme inhibitors in the Survival and Ventricular Enlargement (SAVE) Study. SAVE Investigators[J]. J Am Coll Cardiol, 1997, 29(2): 229-36. doi：10.1016/s0735-1097(96)00489-5
[7]	Dargie HJ. Effect of carvedilol on outcome after myocardial infarction in patients with left-ventricular dysfunction: the CAPRICORN randomised trial[J]. Lancet, 2001, 357(9266): 1385-90. doi：10.1016/s0140-6736(00)04560-8
[8]	Park CS, Yang HM, Ki YJ, et al. Left ventricular ejection fraction 1 year after acute myocardial infarction identifies the benefits of the long-term use of β-blockers: analysis of data from the KAMIR-NIH registry[J]. Circ Cardiovasc Interv, 2021, 14(4): e010159. doi：10.1161/circinterventions.120.010159
[9]	Packer M, Fowler MB, Roecker EB, et al. Effect of carvedilol on the morbidity of patients with severe chronic heart failure: results of the carvedilol prospective randomized cumulative survival (COPERNICUS) study[J]. Circulation, 2002, 106(17): 2194-9. doi：10.1161/01.cir.0000035653.72855.bf
[10]	Virani SS, Newby LK, Arnold SV, et al. 2023 AHA/ACC/ACCP/ASPC/NLA/PCNA guideline for the management of patients with chronic coronary disease: a report of the American heart association/American college of cardiology joint committee on clinical practice guidelines[J]. Circulation, 2023, 148(9): e9-e119. doi：10.1161/cir.0000000000001183
[11]	Vrints C, Andreotti F, Koskinas KC, et al. 2024 ESC Guidelines for the management of chronic coronary syndromes[J]. Eur Heart J, 2024, 45(36): 3415-537.
[12]	中华医学会心血管病学分会, 中华心血管病杂志编辑委员会. 中国慢性冠脉综合征患者诊断及管理指南[J]. 中华心血管病杂志, 2024, 52(6): 589-614.
[13]	Park J, Han JK, Kang J, et al. The clinical impact of β-blocker therapy on patients with chronic coronary artery disease after percutaneous coronary intervention[J]. Korean Circ J, 2022, 52(7): 544-55. doi：10.4070/kcj.2021.0395
[14]	Khan SU, Akbar UA, Khan MS, et al. Beta-blockers after PCI for stable coronary artery disease and preserved left ventricular ejection fraction[J]. JACC Adv, 2025, 4(2): 101566. doi：10.1016/j.jacadv.2024.101566
[15]	Consortium TC, Cao YN, Li L, et al. The ChinaMAP analytics of deep whole genome sequences in 10, 588 individuals[J]. Cell Res, 2020, 30(9): 717-31. doi：10.1038/s41422-020-0322-9
[16]	Hwang MJ. Demographic change in east Asia: cultural legacies, contemporary challenges, and strategic responses[J]. China Popul Dev Stud, 2025, 9(2): 142-50. doi：10.1007/s42379-025-00198-3
[17]	Suzuki S, Hashizume N, Kanzaki Y, et al. Prognostic significance of serum albumin in patients with stable coronary artery disease treated by percutaneous coronary intervention[J]. PLoS One, 2019, 14(7): e0219044. doi：10.1371/journal.pone.0219044
[18]	Kim J, Kang D, Park H, et al. Long-term β‑blocker therapy and clinical outcomes after acute myocardial infarction in patients without heart failure: nationwide cohort study[J]. Eur Heart J, 2020, 41(37): 3521-9. doi：10.1093/eurheartj/ehaa376
[19]	Dahl Aarvik M, Sandven I, Dondo TB, et al. Effect of oral β-blocker treatment on mortality in contemporary post-myocardial infarction patients: a systematic review and meta-analysis[J]. Eur Heart J Cardiovasc Pharmacother, 2019, 5(1): 12-20. doi：10.1093/ehjcvp/pvy034
[20]	Ishak D, Aktaa S, Lindhagen L, et al. Association of beta-blockers beyond 1 year after myocardial infarction and cardiovascular outcomes[J]. Heart, 2023, 109(15): 1159-65. doi：10.1136/heartjnl-2022-322115
[21]	Neumann A, Maura G, Weill A, et al. Clinical events after discontinuation of β‑blockers in patients without heart failure optimally treated after acute myocardial infarction: a cohort study on the French healthcare databases[J]. Circ Cardiovasc Qual Outcomes, 2018, 11(4): e004356. doi：10.1161/circoutcomes.117.004356
[22]	Ibáñez B, Latini R, Rosselló X, et al. Beta-blockers after myocardial infarction without reduced ejection fraction[J]. N Engl J Med, 2025.
[23]	Munkhaugen J, Kristensen AMD, Halvorsen S, et al. Beta-blockers after myocardial infarction in patients without heart failure[J]. N Engl J Med, 2025. .
[24]	Sorbets E, Steg PG, Young R, et al. β-blockers, calcium antagonists, and mortality in stable coronary artery disease: an international cohort study[J]. Eur Heart J, 2019, 40(18): 1399-407. doi：10.1093/eurheartj/ehy811
[25]	Bangalore S, Steg G, Deedwania P, et al. β-Blocker use and clinical outcomes in stable outpatients with and without coronary artery disease[J]. JAMA, 2012, 308(13): 1340-9. doi：10.1001/jama.2012.12559
[26]	Godoy LC, Farkouh ME, Austin PC, et al. Association of beta-blocker therapy with cardiovascular outcomes in patients with stable ischemic heart disease[J]. J Am Coll Cardiol, 2023, 81(24): 2299-311. doi：10.1016/j.jacc.2023.04.021
[27]	应用β肾上腺素能受体阻滞剂规范治疗冠心病的中国专家共识[J]. 中国循环杂志, 2020, 35(02): 108-23.
[28]	Jin P, Ma J, Wu P, et al. PCSK9 inhibition mitigates vulnerable plaque formation induced by hyperhomocysteinemia through regulating lipid metabolism and inflammation[J]. Biochem Pharmacol, 2025, 239: 117031. doi：10.1016/j.bcp.2025.117137
[29]	Biccirè FG, Häner J, Losdat S, et al. Concomitant coronary atheroma regression and stabilization in response to lipid-lowering therapy[J]. J Am Coll Cardiol, 2023, 82(18): 1737-47. doi：10.1016/j.jacc.2023.08.019
[30]	Montalto C, Costa F, Leonardi S, et al. Dual antiplatelet therapy duration after percutaneous coronary intervention in patients with indication to oral anticoagulant therapy. A systematic review and meta-analysis of randomized controlled trials[J]. Eur Heart J Cardiovasc Pharmacother, 2023, 9(3): 220-30. doi：10.1093/ehjcvp/pvac065
[31]	Kereiakes DJ. Dual antiplatelet therapy duration following percutaneous coronary intervention: time for a change[J]. J Soc Cardiovasc Angiogr Interv, 2025, 4(2): 102510. doi：10.1016/j.jscai.2024.102510

Variable	Total (n=204)	Control group (n=149)	β-blocker group (n=55)	Statistic	P
Age (year)	72.6±10.3	72.9±10.1	71.8±11.0	0.416	0.520
Gender [n (%)]				0.060	0.806
Female	62 (30.4)	46 (30.9)	16 (29.1)
Male	142 (69.6)	103 (69.1)	39 (70.9)
Smoking [n (%)]	101 (49.5)	77 (51.7)	24 (43.6)	1.039	0.308
BMI (kg/m²)	23.6±3.9	23.4±3.8	24.3±4.1	2.018	0.157
SBP (mmHg)	136.3±20.4	135.8±19.6	137.5±22.7	0.254	0.615
DBP (mmHg)	77.4±13.2	77.2±12.9	77.9±14.1	0.108	0.743
Hemoglobin (g/dL)	13.6±2.0	13.6±1.9	13.5±2.2	0.037	0.847
Albumin (g/L)	3.9±0.5	3.9±0.5	3.9±0.5	0.167	0.683
eGFR (mL/min/1.73 m²)	61.3±24.6	63.8±24.2	54.7±24.6	5.583	0.019
AST (U/L)	24.7±11.0	25.5±11.6	22.6±8.7	2.841	0.093
ALT (U/L)	20.9±12.2	21.5±12.7	19.5±10.6	1.016	0.315
TC (mg/dL)	185.4±35.7	184.4±35.2	188.4±37.4	0.390	0.533
TG (mg/dL)	117.0 (83.5, 159.5)	118.0 (84.0, 157.0)	105.5 (73.5, 159.8)	1.052	0.305
HDL-C (mg/dL)	50.2±13.2	49.9±13.0	51.1±13.8	0.314	0.576
LDL-C (mg/dL)	110.1±28.5	109.3±28.3	112.1±29.4	0.394	0.531
HbA1C (%)	6.0 (5.7, 6.7)	6.0 (5.6, 6.6)	6.0 (5.7, 7.0)	2.139	0.144
CRP (mg/dL)	0.1 (0.0, 0.3)	0.1 (0.0, 0.3)	0.1 (0.1, 0.3)	1.240	0.266
LVEF (%)	63.2±9.8	65.0±7.3	58.6±13.6	18.205	<0.001
Cerebral infarction [n (%)]	35 (17.2)	27 (18.1)	8 (14.5)	0.361	0.548
Peripheral arterial disease [n (%)]	53 (26.0)	42 (28.2)	11 (20)	1.400	0.237
Atrial fibrillation [n (%)]	26 (12.7)	13 (8.7)	13 (23.6)	8.032	0.005
Hypertension [n (%)]	151 (74.0)	111 (74.5)	40 (72.7)	0.065	0.798
Dyslipidemia [n (%)]	104 (51.0)	78 (52.3)	26 (47.3)	0.414	0.520
Diabetes [n (%)]	73 (35.8)	50 (33.6)	23 (41.8)	1.193	0.275

Variable	Total (n=204)	Control group (n=149)	β-blocker group (n=55)	Statistic	P
Age (year)	72.6±10.3	72.9±10.1	71.8±11.0	0.416	0.520
Gender [n (%)]				0.060	0.806
Female	62 (30.4)	46 (30.9)	16 (29.1)
Male	142 (69.6)	103 (69.1)	39 (70.9)
Smoking [n (%)]	101 (49.5)	77 (51.7)	24 (43.6)	1.039	0.308
BMI (kg/m²)	23.6±3.9	23.4±3.8	24.3±4.1	2.018	0.157
SBP (mmHg)	136.3±20.4	135.8±19.6	137.5±22.7	0.254	0.615
DBP (mmHg)	77.4±13.2	77.2±12.9	77.9±14.1	0.108	0.743
Hemoglobin (g/dL)	13.6±2.0	13.6±1.9	13.5±2.2	0.037	0.847
Albumin (g/L)	3.9±0.5	3.9±0.5	3.9±0.5	0.167	0.683
eGFR (mL/min/1.73 m²)	61.3±24.6	63.8±24.2	54.7±24.6	5.583	0.019
AST (U/L)	24.7±11.0	25.5±11.6	22.6±8.7	2.841	0.093
ALT (U/L)	20.9±12.2	21.5±12.7	19.5±10.6	1.016	0.315
TC (mg/dL)	185.4±35.7	184.4±35.2	188.4±37.4	0.390	0.533
TG (mg/dL)	117.0 (83.5, 159.5)	118.0 (84.0, 157.0)	105.5 (73.5, 159.8)	1.052	0.305
HDL-C (mg/dL)	50.2±13.2	49.9±13.0	51.1±13.8	0.314	0.576
LDL-C (mg/dL)	110.1±28.5	109.3±28.3	112.1±29.4	0.394	0.531
HbA1C (%)	6.0 (5.7, 6.7)	6.0 (5.6, 6.6)	6.0 (5.7, 7.0)	2.139	0.144
CRP (mg/dL)	0.1 (0.0, 0.3)	0.1 (0.0, 0.3)	0.1 (0.1, 0.3)	1.240	0.266
LVEF (%)	63.2±9.8	65.0±7.3	58.6±13.6	18.205	<0.001
Cerebral infarction [n (%)]	35 (17.2)	27 (18.1)	8 (14.5)	0.361	0.548
Peripheral arterial disease [n (%)]	53 (26.0)	42 (28.2)	11 (20)	1.400	0.237
Atrial fibrillation [n (%)]	26 (12.7)	13 (8.7)	13 (23.6)	8.032	0.005
Hypertension [n (%)]	151 (74.0)	111 (74.5)	40 (72.7)	0.065	0.798
Dyslipidemia [n (%)]	104 (51.0)	78 (52.3)	26 (47.3)	0.414	0.520
Diabetes [n (%)]	73 (35.8)	50 (33.6)	23 (41.8)	1.193	0.275

Variable	Total (n=204)	Control group (n=149)	β-blocker group (n=55)	Statistic	P
Coronary angiography status
LMT lesions	13 (6.4)	10 (6.7)	3 (5.5)	-	1.000
Bifurcation lesions	102 (50.0)	70 (47)	32 (58.2)	2.016	0.156
Ostial lesions	30 (14.7)	22 (14.8)	8 (14.5)	0.002	0.969
Calcified lesions	29 (14.2)	21 (14.1)	8 (14.5)	0.007	0.935
CTO lesions	12 (5.9)	9 (6)	3 (5.5)	-	1.000
Multi-vessel lesions	53 (26.0)	38 (25.5)	15 (27.3)	0.065	0.798
Stent				-	0.171
BMS	11 (5.4)	6 (4)	5 (9.1)
DES	193 (94.6)	143 (96)	50 (90.9)
Medication
Aspirin	202 (99.0)	148 (99.3)	54 (98.2)	-	0.467
Thienopiridines	200 (98.0)	147 (98.7)	53 (96.4)	-	0.294
Warfarin	5 (2.5)	2 (1.3)	3 (5.5)	-	0.123
NOAC	21 (10.3)	12 (8.1)	9 (16.4)	3.004	0.083
Ezetimibe	3 (1.5)	3 (2)	0 (0)	-	0.565
PPI	134 (65.7)	104 (69.8)	30 (54.5)	4.147	0.042
Statin	111 (54.4)	86 (57.7)	25 (45.5)	2.436	0.119
ACEI	19 (9.3)	14 (9.4)	5 (9.1)	0.004	0.947
ARB	88 (43.1)	66 (44.3)	22 (40)	0.302	0.583
MRA	11 (5.4)	5 (3.4)	6 (10.9)	-	0.072
Outcomes
All-cause death	18 (8.8)	13 (8.7)	5 (9.1)	-	1.000
MACEs	19 (9.3)	15 (10.1)	4 (7.3)	0.371	0.542
Cardiovascular death	6 (2.9)	4 (2.7)	2 (3.6)	-	0.662
Non-fatal MI	3 (1.5)	3 (2.0)	0 (0.0)	-	0.565
Non-fatal stroke	11 (5.4)	9 (6.0)	2 (3.6)	-	0.731

Variable	Total (n=204)	Control group (n=149)	β-blocker group (n=55)	Statistic	P
Coronary angiography status
LMT lesions	13 (6.4)	10 (6.7)	3 (5.5)	-	1.000
Bifurcation lesions	102 (50.0)	70 (47)	32 (58.2)	2.016	0.156
Ostial lesions	30 (14.7)	22 (14.8)	8 (14.5)	0.002	0.969
Calcified lesions	29 (14.2)	21 (14.1)	8 (14.5)	0.007	0.935
CTO lesions	12 (5.9)	9 (6)	3 (5.5)	-	1.000
Multi-vessel lesions	53 (26.0)	38 (25.5)	15 (27.3)	0.065	0.798
Stent				-	0.171
BMS	11 (5.4)	6 (4)	5 (9.1)
DES	193 (94.6)	143 (96)	50 (90.9)
Medication
Aspirin	202 (99.0)	148 (99.3)	54 (98.2)	-	0.467
Thienopiridines	200 (98.0)	147 (98.7)	53 (96.4)	-	0.294
Warfarin	5 (2.5)	2 (1.3)	3 (5.5)	-	0.123
NOAC	21 (10.3)	12 (8.1)	9 (16.4)	3.004	0.083
Ezetimibe	3 (1.5)	3 (2)	0 (0)	-	0.565
PPI	134 (65.7)	104 (69.8)	30 (54.5)	4.147	0.042
Statin	111 (54.4)	86 (57.7)	25 (45.5)	2.436	0.119
ACEI	19 (9.3)	14 (9.4)	5 (9.1)	0.004	0.947
ARB	88 (43.1)	66 (44.3)	22 (40)	0.302	0.583
MRA	11 (5.4)	5 (3.4)	6 (10.9)	-	0.072
Outcomes
All-cause death	18 (8.8)	13 (8.7)	5 (9.1)	-	1.000
MACEs	19 (9.3)	15 (10.1)	4 (7.3)	0.371	0.542
Cardiovascular death	6 (2.9)	4 (2.7)	2 (3.6)	-	0.662
Non-fatal MI	3 (1.5)	3 (2.0)	0 (0.0)	-	0.565
Non-fatal stroke	11 (5.4)	9 (6.0)	2 (3.6)	-	0.731

Model	All-cause death		MACEs
Model	HR (95% CI)	P	HR (95% CI)	P
Univariate Cox regression	1.08 (0.38-3.04)	0.881	0.73 (0.30-1.81)	0.498
Multivariate Cox regression*	0.81 (0.24-2.72)	0.735	0.62 (0.22-1.69)	0.348
PS adjustment	0.69 (0.21-2.27)	0.542	0.56 (0.20-1.52)	0.255
PS matching	1.49 (0.25-8.91)	0.664	0.59 (0.17-2.10)	0.415
IPTW	0.60 (0.17-2.11)	0.383	0.53 (0.20-1.45)	0.244
SMRW	0.91 (0.33-2.54)	0.881	0.64 (0.26-1.58)	0.386