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澳大利亚成年人队列中心脏代谢风险的连续临床指标的验证。

Validation of continuous clinical indices of cardiometabolic risk in a cohort of Australian adults.

机构信息

Spatial Epidemiology and Evaluation Research Group, School of Population Health and Sansom Institute for Health Research, University of South Australia, Adelaide, South Australia, Australia.

出版信息

BMC Cardiovasc Disord. 2014 Feb 27;14:27. doi: 10.1186/1471-2261-14-27.

Abstract

BACKGROUND

Indicators of cardiometabolic risk typically include non-clinical factors (e.g., smoking). While the incorporation of non-clinical factors can improve absolute risk prediction, it is impossible to study the contribution of non-clinical factors when they are both predictors and part of the outcome measure. Metabolic syndrome, incorporating only clinical measures, seems a solution yet provides no information on risk severity. The aims of this study were: 1) to construct two continuous clinical indices of cardiometabolic risk (cCICRs), and assess their accuracy in predicting 10-year incident cardiovascular disease and/or type 2 diabetes; and 2) to compare the predictive accuracies of these cCICRs with existing risk indicators that incorporate non-clinical factors (Framingham Risk Scores).

METHODS

Data from a population-based biomedical cohort (n = 4056) were used to construct two cCICRs from waist circumference, mean arteriole pressure, fasting glucose, triglycerides and high density lipoprotein: 1) the mean of standardised risk factors (cCICR-Z); and 2) the weighted mean of the two first principal components from principal component analysis (cCICR-PCA). The predictive accuracies of the two cCICRs and the Framingham Risk Scores were assessed and compared using ROC curves.

RESULTS

Both cCICRs demonstrated moderate accuracy (AUCs 0.72 - 0.76) in predicting incident cardiovascular disease and/or type 2 diabetes, among men and women. There were no significant differences between the predictive accuracies of the cCICRs and the Framingham Risk Scores.

CONCLUSIONS

cCICRs may be useful in research investigating associations between non-clinical factors and health by providing suitable alternatives to current risk indicators which include non-clinical factors.

摘要

背景

心血管代谢风险的指标通常包括非临床因素(例如,吸烟)。虽然纳入非临床因素可以提高绝对风险预测的准确性,但当非临床因素既是预测因素又是结果测量的一部分时,就不可能研究非临床因素的贡献。仅包含临床指标的代谢综合征似乎是一种解决方案,但它不能提供关于风险严重程度的信息。本研究的目的是:1)构建两个连续的心血管代谢风险临床指标(cCICR),并评估它们预测 10 年心血管疾病和/或 2 型糖尿病发病的准确性;2)比较这些 cCICR 与包含非临床因素的现有风险指标(弗雷明汉风险评分)的预测准确性。

方法

使用基于人群的生物医学队列(n=4056)的数据,从腰围、平均动脉压、空腹血糖、甘油三酯和高密度脂蛋白中构建两个 cCICR:1)标准化风险因素的平均值(cCICR-Z);2)主成分分析(PCA)的前两个主成分的加权平均值(cCICR-PCA)。使用 ROC 曲线评估和比较两种 cCICR 和弗雷明汉风险评分的预测准确性。

结果

两种 cCICR 在预测男性和女性心血管疾病和/或 2 型糖尿病发病方面均具有中等准确性(AUCs 0.72-0.76)。cCICR 与弗雷明汉风险评分的预测准确性之间没有显著差异。

结论

cCICR 可以在研究非临床因素与健康之间的关联方面发挥作用,为包括非临床因素在内的现有风险指标提供合适的替代方法。

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