Direct factor Xa inhibitors and the risk of cancer and cancer mortality: A Danish population-based cohort study.

IF 15.8 1区 医学 Q1 Medicine PLoS Medicine Pub Date : 2024-07-01 DOI:10.1371/journal.pmed.1004400
Floris Bosch, Erzsébet Horváth-Puhó, Suzanne C Cannegieter, Nick van Es, Henrik T Sørensen
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Abstract

Background: Preclinical animal studies have suggested that myeloid cell-synthesized coagulation factor X dampens antitumor immunity and that rivaroxaban, a direct factor Xa inhibitor, can be used to promote tumor immunity. This study was aimed at assessing whether patients with atrial fibrillation taking direct factor Xa inhibitors have lower risk of cancer and cancer-related mortality than patients taking the direct thrombin inhibitor dabigatran.

Methods and findings: This nationwide population-based cohort study in Denmark included adult patients with atrial fibrillation and without a history of cancer, who started taking a factor Xa inhibitor or dabigatran between 2011 and 2015. Data on medical history, outcomes, and drug use were acquired through Danish healthcare registries. The primary outcome was any cancer. Secondary outcomes were cancer-related mortality and all-cause mortality. Outcome events were assessed during 5 years of follow-up in an intention-to-treat analysis. The propensity score-based inverse probability of treatment weighting was used to compute cumulative incidence and subdistribution hazard ratios (SHRs) and corresponding 95% confidence intervals (CIs), with death as a competing event. Propensity scores were estimated using logistic regression and including in the model sex, age group at index date, comorbidities, and use of comedications. A total of 11,742 patients with atrial fibrillation starting a factor Xa inhibitor and 11,970 patients starting dabigatran were included. Mean age was 75.2 years (standard deviation [SD] 11.2) in the factor Xa cohort and 71.7 years (SD 11.1) in the dabigatran cohort. On the basis of the propensity score-weighted models, after 5 years of follow-up, no substantial difference in the cumulative incidence of cancer was observed between the factor Xa inhibitor (2,157/23,711; 9.11%, 95% CI [8.61%,9.63%]) and dabigatran (2,294/23,715; 9.68%, 95% CI [9.14%,10.25%]) groups (SHR 0.94, 95% CI [0.89,1.00], P value 0.0357). We observed no difference in cancer-related mortality (factor Xa inhibitors cohort 1,028/23,711; 4.33%, 95% CI [4.02%,4.68%]. Dabigatran cohort 1,001/23,715; 4.22%, 95% CI [3.83%,4.66%]; SHR 1.03, 95% CI [0.94,1.12]), but all-cause mortality was higher in the factor Xa inhibitor cohort (factor Xa inhibitors cohort 7,416/23,711; 31.31%, 95% CI [30.37%,32.29%]. Dabigatran cohort 6,531/23,715; 27.56%, 95% CI [26.69%,28.45%]; HR 1.17, 95% CI [1.13,1.21]). The main limitations of the study were the possibility of residual confounding and the short follow-up period.

Conclusions: In this population based cohort study, factor Xa inhibitor use was not associated with an overall lower incidence of cancer or cancer-related mortality when compared to dabigatran. We did observe an increase in all-cause mortality in the factor Xa inhibitor cohort.

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Xa 直接因子抑制剂与癌症风险和癌症死亡率:一项基于丹麦人口的队列研究。
背景:临床前动物实验表明,骨髓细胞合成的凝血因子X会抑制抗肿瘤免疫,而利伐沙班(一种直接Xa因子抑制剂)可用于促进肿瘤免疫。本研究旨在评估与服用直接凝血酶抑制剂达比加群的患者相比,服用直接Xa因子抑制剂的心房颤动患者罹患癌症的风险和癌症相关死亡率是否更低:这项基于丹麦全国人口的队列研究纳入了2011年至2015年间开始服用Xa因子抑制剂或达比加群且无癌症病史的成年心房颤动患者。有关病史、疗效和药物使用的数据均通过丹麦医疗登记处获得。主要结果是任何癌症。次要结果为癌症相关死亡率和全因死亡率。在意向治疗分析中,对随访 5 年的结果事件进行了评估。采用基于倾向评分的治疗逆概率加权法计算累计发病率和亚分布危险比 (SHR) 以及相应的 95% 置信区间 (CI),并将死亡作为竞争事件。采用逻辑回归法估算倾向评分,并将性别、发病日期的年龄组别、合并症和合并用药纳入模型。共纳入了11742名开始使用Xa因子抑制剂的心房颤动患者和11970名开始使用达比加群的患者。Xa 因子队列的平均年龄为 75.2 岁(标准差 [SD] 11.2),达比加群队列的平均年龄为 71.7 岁(标准差 11.1)。根据倾向得分加权模型,随访 5 年后,Xa 因子抑制剂与达比加群间的癌症累积发病率没有实质性差异(2 157/23 711;9.11%,95% CI [8.61%,9.63%])和达比加群(2,294/23,715;9.68%,95% CI [9.14%,10.25%])组之间没有观察到实质性差异(SHR 0.94,95% CI [0.89,1.00],P 值 0.0357)。我们观察到癌症相关死亡率没有差异(Xa因子抑制剂队列 1,028/23,711; 4.33%,95% CI [4.02%,4.68%]。达比加群 1,001/23,715; 4.22%, 95% CI [3.83%,4.66%]; SHR 1.03, 95% CI [0.94,1.12]),但 Xa 因子抑制剂队列的全因死亡率较高(Xa 因子抑制剂队列 7,416/23,711; 31.31%, 95% CI [30.37%,32.29%].达比加群 6,531/23,715; 27.56%, 95% CI [26.69%,28.45%]; HR 1.17, 95% CI [1.13,1.21])。研究的主要局限性在于可能存在残余混杂因素和随访时间较短:在这项基于人群的队列研究中,与达比加群相比,Xa因子抑制剂的使用与癌症或癌症相关死亡率的总体降低无关。我们确实观察到 Xa 因子抑制剂队列中的全因死亡率有所上升。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
PLoS Medicine
PLoS Medicine MEDICINE, GENERAL & INTERNAL-
CiteScore
17.60
自引率
0.60%
发文量
227
审稿时长
4-8 weeks
期刊介绍: PLOS Medicine is a prominent platform for discussing and researching global health challenges. The journal covers a wide range of topics, including biomedical, environmental, social, and political factors affecting health. It prioritizes articles that contribute to clinical practice, health policy, or a better understanding of pathophysiology, ultimately aiming to improve health outcomes across different settings. The journal is unwavering in its commitment to uphold the highest ethical standards in medical publishing. This includes actively managing and disclosing any conflicts of interest related to reporting, reviewing, and publishing. PLOS Medicine promotes transparency in the entire review and publication process. The journal also encourages data sharing and encourages the reuse of published work. Additionally, authors retain copyright for their work, and the publication is made accessible through Open Access with no restrictions on availability and dissemination. PLOS Medicine takes measures to avoid conflicts of interest associated with advertising drugs and medical devices or engaging in the exclusive sale of reprints.
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