新西兰初级保健中14000多名癌症幸存者的心血管疾病风险预测方程的性能:一项验证研究
Performance of cardiovascular disease risk prediction equations in more than 14 000 survivors of cancer in New Zealand primary care: a validation study.
作者信息
Tawfiq Essa, Selak Vanessa, Elwood J Mark, Pylypchuk Romana, Tin Sandar Tin, Harwood Matire, Grey Corina, McKeage Mark, Wells Sue
机构信息
School of Population Health, University of Auckland, Auckland, New Zealand.
School of Population Health, University of Auckland, Auckland, New Zealand.
出版信息
Lancet. 2023 Feb 4;401(10374):357-365. doi: 10.1016/S0140-6736(22)02405-9. Epub 2023 Jan 23.
BACKGROUND
People with cancer have an increased risk of cardiovascular disease. Risk prediction equations developed in New Zealand accurately predict 5-year cardiovascular disease risk in a general primary care population in the country. We assessed the performance of these equations for survivors of cancer in New Zealand.
METHODS
For this validation study, patients aged 30-74 years from the PREDICT open cohort study, which was used to develop the New Zealand cardiovascular disease risk prediction equations, were included in the analysis if they had a primary diagnosis of invasive cancer at least 2 years before the date of the first cardiovascular disease risk assessment. The risk prediction equations are sex-specific and include the following predictors: age, ethnicity, socioeconomic deprivation index, family history of cardiovascular disease, smoking status, history of atrial fibrillation and diabetes, systolic blood pressure, total cholesterol to HDL cholesterol ratio, and preventive pharmacotherapy (blood-pressure-lowering, lipid-lowering, and antithrombotic drugs). Calibration was assessed by comparing the mean predicted 5-year cardiovascular disease risk, estimated using the risk prediction equations, with the observed risk across deciles of risk, for men and women, and according to the three clinical 5-year cardiovascular disease risk groups in New Zealand guidelines (<5%, 5% to <15%, and ≥15%). Discrimination was assessed by Harrell's C statistic.
FINDINGS
14 263 patients were included in the study. The mean age was 61 years (SD 9) for men and 60 years (SD 8) for women, with a median follow-up of 5·8 years for men and 5·7 years for women. The observed cardiovascular disease risk was underpredicted by a maximum of 2·5% in male and 3·2% in female decile groups. When patients were grouped according to clinical risk groups, observed cardiovascular disease risk was underpredicted by less than 2% in the lower risk groups and overpredicted by 2·2% for men and 3·3% for women in the highest risk group. Harrell's C statistics were 0·67 (SE 0·01) for men and 0·73 (0·01) for women.
INTERPRETATION
The New Zealand cardiovascular disease risk prediction equations reasonably predicted the observed 5-year cardiovascular disease risk in survivors of cancer in the country, in whom risk prediction was considered clinically appropriate. Prediction could be improved by adding cancer-specific variables and considering competing risks. Our findings suggest that the equations are reasonable clinical tools for use in survivors of cancer in New Zealand.
FUNDING
Auckland Medical Research Foundation, Health Research Council of New Zealand.
背景
癌症患者患心血管疾病的风险增加。在新西兰开发的风险预测方程能够准确预测该国普通初级保健人群的5年心血管疾病风险。我们评估了这些方程在新西兰癌症幸存者中的预测性能。
方法
在这项验证研究中,来自PREDICT开放队列研究的30-74岁患者被纳入分析,该队列研究用于开发新西兰心血管疾病风险预测方程,条件是他们在首次进行心血管疾病风险评估之日前至少2年被初步诊断为浸润性癌症。风险预测方程是针对特定性别的,包括以下预测因素:年龄、种族、社会经济剥夺指数、心血管疾病家族史、吸烟状况、心房颤动和糖尿病病史、收缩压、总胆固醇与高密度脂蛋白胆固醇之比以及预防性药物治疗(降压药、降脂药和抗血栓药物)。通过比较使用风险预测方程估计的平均预测5年心血管疾病风险与不同风险十分位数组中观察到的风险,对男性和女性进行校准,并根据新西兰指南中的三个临床5年心血管疾病风险组(<5%、5%至<15%和≥15%)进行校准。通过Harrell's C统计量评估辨别力。
结果
14263名患者被纳入研究。男性的平均年龄为61岁(标准差9),女性为60岁(标准差8);男性的中位随访时间为5.8年,女性为5.7年。在男性和女性十分位数组中,观察到的心血管疾病风险最高被低估2.5%和3.2%。当根据临床风险组对患者进行分组时,在低风险组中观察到的心血管疾病风险被低估不到2%,而在高风险组中,男性被高估2.2%,女性被高估3.3%。男性的Harrell's C统计量为0.67(标准误0.0),女性为0.73(0.01)。
解读
新西兰心血管疾病风险预测方程合理地预测了该国癌症幸存者中观察到的5年心血管疾病风险,在这些患者中,风险预测被认为在临床上是合适的。通过添加癌症特异性变量和考虑竞争风险,可以改善预测。我们的研究结果表明,这些方程是用于新西兰癌症幸存者的合理临床工具。
资助
奥克兰医学研究基金会、新西兰健康研究委员会。
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