British Columbia Centre for Disease Control, Vancouver, BC, Canada.
School of Population and Public Health, University of British Columbia, Vancouver, BC, Canada.
J Viral Hepat. 2020 Aug;27(8):781-793. doi: 10.1111/jvh.13295. Epub 2020 Apr 17.
We evaluated the effect of sustained virologic response (SVR) from direct-acting antiviral (DAA)- and interferon-based treatments on hepatocellular carcinoma (HCC) risk in a large population-based cohort in Canada. We used data from the BC Hepatitis Testers Cohort, which includes ~1.3 million individuals tested for HCV since 1990, linked with healthcare administrative and registry datasets. Patients were followed from the end of HCV treatment to HCC, death or 31 December 2016. We assessed HCC risk among those who did and did not achieve SVR by treatment type using proportional hazard models. Of 12 776 eligible individuals, 3905 received DAAs while 8871 received interferon-based treatments, followed for a median of 1.0 [range: 0.6-2.7] and 7.9 [range: 4.4-17.1] years, respectively. A total of 3613 and 6575 achieved SVR with DAAs- and interferon-based treatments, respectively. Among DAAs-treated patients, HCC incidence rate was 6.9 (95%CI: 4.7-10.1)/1000 person yr (PY) in SVR group (HCC cases: 26) and 38.2 (95%CI: 20.6-71.0) in the no-SVR group (HCC cases: 10, P < .001). Among interferon-treated individuals, HCC incidence rate was 1.8 (95%CI: 1.5-2.2) in the SVR (HCC cases: 99) and 13.9 (95%CI: 12.3-15.8) in the no-SVR group (HCC cases: 239, P < .001). Compared with no-SVR from interferon, SVR from DAA- and interferon-based treatments resulted in significant reduction in HCC risk (adjusted subdistribution hazard ratio (adjSHR) DAA = 0.30, 95%CI: 0.19-0.48 and adjSHR interferon = 0.2, 95%CI: 0.16-0.26). Among those with SVR, treatment with DAAs compared to interferon was not associated with HCC risk (adjSHR = 0.93, 95%CI: 0.51-1.71). In conclusion, similar to interferon era, DAA-related SVR is associated with 70% reduction in HCC risk.
我们在加拿大的一个大型基于人群的队列中评估了直接作用抗病毒(DAA)和基于干扰素的治疗的持续病毒学应答(SVR)对肝细胞癌(HCC)风险的影响。我们使用了来自不列颠哥伦比亚省肝炎检测者队列的数据,该队列包括自 1990 年以来接受 HCV 检测的约 130 万人,与医疗保健管理和登记数据集相关联。患者从 HCV 治疗结束到 HCC、死亡或 2016 年 12 月 31 日进行随访。我们使用比例风险模型评估了按治疗类型在获得和未获得 SVR 的患者中 HCC 风险。在 12776 名合格患者中,3905 名接受了 DAA 治疗,8871 名接受了基于干扰素的治疗,中位随访时间分别为 1.0 [范围:0.6-2.7] 和 7.9 [范围:4.4-17.1] 年。共有 3613 名和 6575 名接受 DAA-和基于干扰素的治疗的患者分别获得了 SVR。在 DAA 治疗的患者中,SVR 组的 HCC 发病率为 6.9(95%CI:4.7-10.1)/1000 人年(PY)(HCC 病例:26 例),无 SVR 组为 38.2(95%CI:20.6-71.0)(HCC 病例:10 例,P<.001)。在接受干扰素治疗的个体中,SVR 组的 HCC 发病率为 1.8(95%CI:1.5-2.2)(HCC 病例:99 例),无 SVR 组为 13.9(95%CI:12.3-15.8)(HCC 病例:239 例,P<.001)。与干扰素的无 SVR 相比,DAA-和基于干扰素的治疗的 SVR 可显著降低 HCC 风险(调整后的亚分布风险比(adjSHR)DAA=0.30,95%CI:0.19-0.48 和 adjSHR 干扰素=0.2,95%CI:0.16-0.26)。在获得 SVR 的患者中,与干扰素相比,DAA 治疗与 HCC 风险无关(adjSHR=0.93,95%CI:0.51-1.71)。总之,与干扰素时代相似,DAA 相关的 SVR 与 HCC 风险降低 70%相关。
