胆固醇和炎症双重残余风险对心血管疾病患者全因死亡率的影响。
Effect of dual residual risk of cholesterol and inflammation on all-cause mortality in patients with cardiovascular disease.
机构信息
School of Public Health, North China University of Science and Technology, No. 21 Bohai Road, Caofeidian Eco-city, Tangshan, 063210, Hebei, China.
Hebei Key Laboratory for Chronic Diseases, Tangshan Key Laboratory for Preclinical and Basic Research On Chronic Diseases, School of Basic Medical Sciences, North China University of Science and Technology, No. 21 Bohai Road, Caofeidian Eco-city, Tangshan, 063210, Hebei, China.
出版信息
Cardiovasc Diabetol. 2023 Apr 24;22(1):96. doi: 10.1186/s12933-023-01826-3.
BACKGROUND
Randomized controlled trials confirm that risks of residual cholesterol and residual inflammation remains in patients with cardiovascular disease (CVD) even after lipid-lowering therapy. This study aims to investigate the association between dual residual risk of cholesterol and inflammation and all-cause mortality in a real-world population with CVD.
METHODS
Patients with a CVD history who first took statins between 1 January 2010 and 31 December 2017 in the Kailuan Study were selected as study participants. According to low-density lipoprotein cholesterol (LDL-C) and hypersensitive C-reactive protein levels, patients were divided into those with no residual risk, residual inflammatory risk (RIR), residual cholesterol risk (RCR), and residual cholesterol and inflammatory risk (RCIR). Cox proportional hazard model was conducted to determine hazard ratio (HR) of all-cause mortality for RIR, RCR, and RCIR. Stratified analysis was conducted according to good medication adherence and 75% of the percentage LDL-C decline, high SMART 2 risk score, and blood pressure and blood glucose at standard levels.
RESULTS
After 6.10 years of follow-up, 377 all-cause deaths occurred in 3509 participants (mean age 63.69 ± 8.41 years, 86.78% men). After adjusting for related risk factors, the HR and (95% confidence interval [CI]) of all-cause mortality in the RIR, RCR, and RCIR was 1.63 (1.05, 2.52), 1.37 (0.98, 1.90), and 1.75 (1.25, 2.46), compared with no residual risk. Similar associations were observed in participants with moderate or low statin compliance, a lower percentage of LDL-C decline, high SMART 2 risk score, uncontrolled blood pressure, and uncontrolled blood glucose, in the RCIR had a 1.66-fold, 2.08-fold, 1.69-fold, 2.04-fold, and 2.05-fold higher risk of all-cause mortality, respectively, than the reference.
CONCLUSION
Risks of residual cholesterol and residual inflammation remain in patients with CVD after receiving statins, and their combined effect significantly increases the risk of all-cause mortality. Here, this increased risk was dependent on statin compliance, LDL-C reduction, SMART 2 risk score, and blood pressure and blood glucose control.
背景
随机对照试验证实,即使在降脂治疗后,心血管疾病(CVD)患者仍存在残余胆固醇和残余炎症的风险。本研究旨在探讨 CVD 患者中胆固醇和炎症双重残余风险与全因死亡率之间的关系。
方法
选择 2010 年 1 月 1 日至 2017 年 12 月 31 日期间首次服用他汀类药物的 Kailuan 研究中的 CVD 病史患者作为研究对象。根据低密度脂蛋白胆固醇(LDL-C)和超敏 C 反应蛋白水平,将患者分为无残余风险、残余炎症风险(RIR)、残余胆固醇风险(RCR)和残余胆固醇和炎症风险(RCIR)。采用 Cox 比例风险模型确定 RIR、RCR 和 RCIR 的全因死亡率的危险比(HR)。根据良好的用药依从性和 LDL-C 降低百分比达到 75%、SMART 2 风险评分高以及血压和血糖达标进行分层分析。
结果
经过 6.10 年的随访,3509 名患者中发生 377 例全因死亡(平均年龄 63.69±8.41 岁,86.78%为男性)。在校正相关危险因素后,RIR、RCR 和 RCIR 的全因死亡率 HR(95%置信区间[CI])分别为 1.63(1.05,2.52)、1.37(0.98,1.90)和 1.75(1.25,2.46),与无残余风险相比。在他汀类药物依从性中等或低、LDL-C 降低百分比较低、SMART 2 风险评分高、血压控制不佳和血糖控制不佳的患者中,RCIR 的全因死亡率风险分别比参照组高 1.66 倍、2.08 倍、1.69 倍、2.04 倍和 2.05 倍。
结论
他汀类药物治疗后,CVD 患者仍存在残余胆固醇和残余炎症的风险,两者的联合作用显著增加全因死亡率的风险。在这里,这种风险的增加取决于他汀类药物的依从性、LDL-C 降低、SMART 2 风险评分以及血压和血糖的控制。
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