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抗逆转录病毒治疗起始后,丙型肝炎治愈对 HIV 感染者死亡率和发病率的影响。

Impact of hepatitis C cure on risk of mortality and morbidity in people with HIV after antiretroviral therapy initiation.

机构信息

University Bordeaux, INSERM, Institut Bergonié, BPH, U1219, CIC-EC 1401, Bordeaux.

INRIA SISTM Team, Talence, France.

出版信息

AIDS. 2023 Aug 1;37(10):1573-1581. doi: 10.1097/QAD.0000000000003594. Epub 2023 May 9.

Abstract

OBJECTIVE

Hepatitis C virus (HCV) co-infection is associated with increased morbidity and mortality in people with HIV (PWH). Sustained virological response (SVR) decreases the risk of HCV-associated morbidity. We compared mortality, risk of AIDS-defining events, and non-AIDS nonliver (NANL) cancers between HCV-co-infected PWH who reached SVR and mono-infected PWH.

DESIGN

Adult PWH from 21 cohorts in Europe and North America that collected HCV treatment data were eligible if they were HCV-free at the time of ART initiation.

METHODS

Up to 10 mono-infected PWH were matched (on age, sex, date of ART start, HIV acquisition route, and being followed at the time of SVR) to each HCV-co-infected PWH who reached SVR. Cox models were used to estimate relative hazards (hazard ratio) of all-cause mortality, AIDS-defining events, and NANL cancers after adjustment.

RESULTS

Among 62 495 PWH, 2756 acquired HCV, of whom 649 reached SVR. For 582 of these, at least one mono-infected PWH could be matched, producing a total of 5062 mono-infected PWH. The estimated hazard ratios comparing HCV-co-infected PWH who reached SVR with mono-infected PWH were 0.29 [95% confidence interval (CI) 0.12-0.73] for mortality, 0.85 [0.42-1.74] for AIDS-defining events, and 1.21 [0.86-1.72] for NANL cancer.

CONCLUSION

PWH who reached SVR a short time after HCV acquisition were not at higher risk of overall mortality compared with mono-infected PWH. However, the apparent higher risk of NANL cancers in HCV-co-infected PWH who reached SVR after a DAA-based treatment compared with mono-infected PWH, though compatible with a null association, suggests a need for monitoring of those events following SVR.

摘要

目的

丙型肝炎病毒(HCV)合并感染与艾滋病毒(HIV)感染者(PWH)的发病率和死亡率增加相关。持续病毒学应答(SVR)降低了与 HCV 相关发病率的风险。我们比较了达到 SVR 的 HCV 合并感染 PWH 与单纯感染 PWH 之间的死亡率、发生艾滋病定义事件的风险和非艾滋病非肝脏(NANL)癌症的风险。

设计

来自欧洲和北美的 21 个队列的成年 PWH,如果他们在开始接受抗逆转录病毒治疗(ART)时无 HCV 感染,则有资格入组。

方法

对于每一位达到 SVR 的 HCV 合并感染 PWH,我们匹配了最多 10 位单纯感染 PWH(按年龄、性别、ART 开始日期、HIV 获得途径和在达到 SVR 时的随访情况进行匹配)。使用 Cox 模型调整后估计全因死亡率、艾滋病定义事件和 NANL 癌症的相对危险度(危险比)。

结果

在 62495 名 PWH 中,有 2756 名感染了 HCV,其中 649 名达到了 SVR。对于其中的 582 名,至少可以匹配一名单纯感染 PWH,总共产生了 5062 名单纯感染 PWH。与达到 SVR 的 HCV 合并感染 PWH 相比,比较达到 SVR 的 HCV 合并感染 PWH 与单纯感染 PWH 的估计危险比为:死亡率为 0.29(95%置信区间 [CI] 0.12-0.73)、艾滋病定义事件为 0.85(0.42-1.74)和 NANL 癌症为 1.21(0.86-1.72)。

结论

与单纯感染 PWH 相比,在 HCV 获得后不久达到 SVR 的 PWH 总体死亡率没有更高的风险。然而,与单纯感染 PWH 相比,在接受基于 DAA 的治疗后达到 SVR 的 HCV 合并感染 PWH 中,NANL 癌症的风险似乎更高,尽管与零关联一致,但这表明需要在 SVR 后监测这些事件。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/71b8/11701241/e16befb298af/nihms-2042568-f0001.jpg

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