使用标准心血管风险计算器预测氟嘧啶化疗的心血管事件。
Predicting cardiovascular events with fluoropyrimidine chemotherapy using a standard cardiovascular risk calculator.
机构信息
Barts Heart Centre, Barts Health NHS Trust, London, UK.
Institute of Cardiovascular Science, University College London, London, UK.
出版信息
ESC Heart Fail. 2024 Oct;11(5):3041-3051. doi: 10.1002/ehf2.14879. Epub 2024 Jun 6.
AIMS
Fluoropyrimidine chemotherapy is important for treatment of many solid tumours but is associated with cardiotoxicity. The relationship of fluoropyrimidine-associated cardiotoxicity (FAC) with conventional cardiovascular (CV) risk factors is poorly understood, and standard cardiovascular risk scores are not validated in this context.
METHODS AND RESULTS
Single-centre retrospective study of patients treated with fluoropyrimidine chemotherapy using electronic health records for cardiovascular risk factors (and calculation of QRISK3 score), cancer treatment, and clinical outcomes. FAC was defined by cardiovascular events during or within 3 months of fluoropyrimidine treatment, and Cox regression was used to assess associations of CV risk and cancer treatment with FAC. One thousand eight hundred ninety-eight patients were included (45% male; median age 64 years), with median follow up 24.5 (11.5-48.3 months); 52.7% of patients were at moderate or high baseline CV risk (QRISK3 score >10%) Cardiovascular events occurred in 3.1% (59/1898)-most commonly angina (64.4%, 38/59) and atrial fibrillation (13.6%, 8/59), with 39% events during cycle one of treatment. In univariable analysis, QRISK3 score >20% was significantly associated with incident FAC (HR 2.25, 95% CI 1.11-4.93, P = 0.03). On multivariable analysis, beta-blocker use (HR 1.04, 95% CI 1.00-1.08, P = 0.04) and higher BMI (HR 2.33, 95% CI 1.04-5.19, P = 0.04) were independently associated with incident CV events. Thirty-two of the 59 patients with FAC were subsequently rechallenged with fluoropyrimidine chemotherapy, with repeat CV events in 6% (2/32). Incident FAC did not affect overall survival (P = 0.50).
CONCLUSIONS
High BMI and use of beta-blockers are associated with risk of CV events during fluoropyrimidine chemotherapy. QRISK3 score may also play a role in identifying patients at high risk of CV events during fluoropyrimidine chemotherapy. Re-challenge with further fluoropyrimidine chemotherapy can be considered in patients following CV events during prior treatment.
目的
氟嘧啶化疗对治疗许多实体瘤非常重要,但与心脏毒性有关。氟嘧啶相关心脏毒性(FAC)与传统心血管(CV)危险因素的关系尚未得到很好的理解,并且标准心血管风险评分在这种情况下未得到验证。
方法和结果
使用电子病历对接受氟嘧啶化疗的患者进行了单中心回顾性研究,记录了心血管危险因素(并计算了 QRISK3 评分)、癌症治疗和临床结局。FAC 定义为氟嘧啶治疗期间或治疗后 3 个月内发生心血管事件,并使用 Cox 回归评估 CV 风险和癌症治疗与 FAC 的相关性。共纳入 1898 例患者(45%为男性;中位年龄 64 岁),中位随访时间为 24.5(11.5-48.3 个月);52.7%的患者基线 CV 风险较高(QRISK3 评分>10%)。心血管事件发生率为 3.1%(59/1898),最常见的是心绞痛(64.4%,38/59)和心房颤动(13.6%,8/59),39%的事件发生在治疗的第 1 周期。单变量分析中,QRISK3 评分>20%与 FAC 发生率显著相关(HR 2.25,95%CI 1.11-4.93,P=0.03)。多变量分析显示,β受体阻滞剂的使用(HR 1.04,95%CI 1.00-1.08,P=0.04)和较高的 BMI(HR 2.33,95%CI 1.04-5.19,P=0.04)与 CV 事件的发生独立相关。59 例 FAC 中有 32 例随后再次接受氟嘧啶化疗,再次发生 CV 事件的有 6%(2/32)。FAC 事件的发生并不影响总生存率(P=0.50)。
结论
高 BMI 和β受体阻滞剂的使用与氟嘧啶化疗期间 CV 事件的风险相关。QRISK3 评分也可能在识别氟嘧啶化疗期间 CV 事件风险较高的患者方面发挥作用。在先前治疗中发生 CV 事件后,可考虑再次接受氟嘧啶化疗。
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