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Metformin and risk of hepatocellular carcinoma in patients with type 2 diabetes

机译:二甲双胍和2型糖尿病患者肝细胞癌的风险

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摘要

Abstract Background Whether metformin may reduce hepatocellular carcinoma ( HCC ) risk requires confirmation. Methods Type 2 diabetes patients newly diagnosed during 1999‐2005 and with 2 or more prescriptions of antidiabetic drugs were enrolled from the Taiwan’s National Health Insurance database. A total of 173?917 ever‐users and 21?900 never‐users of metformin were identified (unmatched cohort). A 1:1 matched‐pair cohort of 21?900 ever‐users and 21?900 never‐users based on a propensity score ( PS ) was created. Hazard ratios were estimated by Cox regression incorporated with the inverse probability of treatment weighting using the PS . In addition, interactions with aspirin and statin were evaluated. Results In the unmatched cohort, 619 never‐users and 2642 ever‐users developed HCC , with a respective incidence of 668.0 and 330.7 per 100?000 person‐years and an overall hazard ratio of 0.49 (95% confidence interval: 0.45‐0.54). The hazard ratios for the first (25.7?months), second (25.7‐56.9?months) and third (56.9?months) tertile of cumulative duration of metformin therapy were 0.89 (0.81‐0.98), 0.50 (0.46‐0.56) and 0.23 (0.21‐0.26) respectively. Analyses of the matched cohort showed an overall hazard ratio of 0.76 (0.67‐0.85), and the hazard ratios for the respective tertiles were 1.39 (1.19‐1.62), 0.77 (0.65‐0.91) and 0.37 (0.30‐0.45). Aspirin and statin were observed to have a significant interaction with metformin. Conclusions Metformin was associated with a reduced risk of HCC in a dose‐response pattern. Users of both metformin and aspirin or metformin and statin had the lowest risk.
机译:摘要背景是否二甲双胍可以减少肝细胞癌(HCC)风险需要确认。方法299-2005期间新诊断患者2型糖尿病患者,并从台湾全国医疗保险数据库中注册了2种或更多的抗糖尿病药物处方。共有173岁?917岁的用户和21?900欧元的二甲双胍(无与伦比的群组)。 A 1:1匹配的一对队列21?900用户和21?900 Neul-User基于倾向评分(PS)。通过COX回归估计危害比率,其掺入使用PS的治疗加权的反概率。此外,评估与阿司匹林和汀类蛋白的相互作用。结果无与伦比的队列,619名从不用户和2642名用户开发的HCC,每100 000人的相应入射668.0和330.7,总体危险比为0.49(95%置信区间:0.45-0.54) 。第一个(25.7?个月)的危险比,第二(25.7-56.9?月)和第三(& 56.9?月)累积的二甲双胍治疗的持续时间为0.89(0.81-0.98),0.50(0.46- 0.56)和0.23(0.21-0.26)。匹配队列的分析显示为0.76(0.67-0.85)的整体危险比,各乳液的危险比为1.39(1.19-1.62),0.77(0.65-0.91)和0.37(0.30-0.45)。观察到阿司匹林和他汀类蛋白与二甲双胍具有显着的相互作用。结论二甲双胍在剂量 - 反应模式下与HCC的风险降低有关。二甲双胍和阿司匹林或二甲双胍和他汀类药物的用户风险最低。

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