The interaction between triglyceride-glucose index and visceral adiposity in cardiovascular disease risk: findings from a nationwide Chinese cohort.

IF 8.5 1区 医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS
Yuhao Yang, Shengxi Li, Qiao Ren, Yu Qiu, Mengjia Pan, Guanglei Liu, Rise Zheng, Zhenmei An, Shuangqing Li
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引用次数: 0

Abstract

Background: Globally, cardiovascular disease (CVD) constitutes the primary cause of death, with insulin resistance (IR), measured by the triglyceride-glucose (TyG) index, and visceral obesity, reflected by the Chinese Visceral Adiposity Index (CVAI), as key contributors. However, the relationship between the TyG index and CVAI regarding CVD risk remains insufficiently understood. This research investigates the interactive impact of the TyG index and CVAI on the risk of cardiovascular disease.

Methods: We analyzed data from 8,358 participants from the China Health and Retirement Longitudinal Study (CHARLS) over a 9-year follow-up period. Participants were classified into four groups based on median TyG index (8.59) and CVAI values (101.26), and baseline characteristics were summarized. Missing data were addressed using multiple imputation by chained equations (MICE). Cox proportional hazards models assessed associations between TyG index, CVAI, CVD, coronary heart disease (CHD), and stroke risks, with Kaplan-Meier analysis used for cumulative hazard. Interaction effects were evaluated using both multiplicative and additive measures. Subgroup analyses by age, gender, and clinical conditions were conducted to explore interaction effects across different populations. Sensitivity analyses re-tested models, excluding the covariates BMI and diabetes, using tertiles for classification, and re-evaluating imputed data.

Results: Over the 9-year follow-up, 1,240 participants (14.8%) developed CVD, including 896 cases of CHD and 475 strokes. Kaplan-Meier curves indicated that participants with low TyG index but high CVAI had the highest cumulative hazard of CVD. Cox regression showed that this group had the highest CVD risk (HR = 1.87, 95% CI: 1.57-2.24), followed by those with both high TyG index and high CVAI (HR = 1.75, 95% CI: 1.49-2.06). Interaction analysis revealed a negative interaction effect between high TyG and high CVAI on CVD and CHD risks, with no significant effect on stroke. Subgroup and sensitivity analyses further confirmed these findings, showing consistent results across demographic groups and under various analytical conditions.

Conclusion: This study suggests that the interaction between IR (TyG index) and visceral fat accumulation (CVAI) plays a complex role in CVD risk, with a potential antagonistic effect observed between high TyG and high CVAI on CVD events. These findings highlight the importance of considering both IR and visceral adiposity in CVD risk assessments to improve the identification of high-risk individuals.

甘油三酯-葡萄糖指数与内脏脂肪在心血管疾病风险中的相互作用:来自中国全国性队列的研究结果。
背景:在全球范围内,心血管疾病(CVD)是导致死亡的主要原因,而以甘油三酯-葡萄糖(TyG)指数衡量的胰岛素抵抗(IR)和以中国内脏脂肪指数(CVAI)反映的内脏肥胖是导致心血管疾病的主要因素。然而,TyG 指数和 CVAI 之间关于心血管疾病风险的关系仍未得到充分了解。本研究探讨了TyG指数和CVAI对心血管疾病风险的交互影响:我们分析了中国健康与退休纵向研究(CHARLS)8358 名参与者在 9 年随访期内的数据。根据中位 TyG 指数(8.59)和 CVAI 值(101.26)将参与者分为四组,并总结了基线特征。缺失数据通过链式方程(MICE)进行多重估算。Cox比例危险度模型评估了TyG指数、CVAI、心血管疾病、冠心病(CHD)和中风风险之间的关联,累积危险度采用Kaplan-Meier分析法。采用乘法和加法评估了交互效应。按年龄、性别和临床条件进行了分组分析,以探讨不同人群的交互效应。敏感性分析对模型进行了重新测试,排除了协变量体重指数(BMI)和糖尿病,使用三等分进行分类,并重新评估了估算数据:在为期 9 年的随访中,1240 名参与者(14.8%)患上了心血管疾病,其中包括 896 例冠心病和 475 例脑卒中。Kaplan-Meier 曲线显示,TyG 指数低但 CVAI 高的参与者患心血管疾病的累积风险最高。Cox回归显示,该组人群的心血管疾病风险最高(HR = 1.87,95% CI:1.57-2.24),其次是TyG指数高和CVAI高的人群(HR = 1.75,95% CI:1.49-2.06)。交互作用分析显示,高TyG指数和高CVAI对心血管疾病和冠心病风险有负交互作用,而对中风无显著影响。亚组分析和敏感性分析进一步证实了这些结果,显示出不同人口群体和不同分析条件下的结果一致:本研究表明,IR(TyG 指数)和内脏脂肪堆积(CVAI)之间的相互作用在心血管疾病风险中起着复杂的作用,高 TyG 和高 CVAI 对心血管疾病事件有潜在的拮抗作用。这些发现凸显了在心血管疾病风险评估中同时考虑IR和内脏脂肪的重要性,以提高对高危人群的识别能力。
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来源期刊
Cardiovascular Diabetology
Cardiovascular Diabetology 医学-内分泌学与代谢
CiteScore
12.30
自引率
15.10%
发文量
240
审稿时长
1 months
期刊介绍: Cardiovascular Diabetology is a journal that welcomes manuscripts exploring various aspects of the relationship between diabetes, cardiovascular health, and the metabolic syndrome. We invite submissions related to clinical studies, genetic investigations, experimental research, pharmacological studies, epidemiological analyses, and molecular biology research in this field.
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