冈比亚未经治疗的成年慢性乙型肝炎患者的临床疗效:前瞻性 PROLIFICA 队列研究数据分析

IF 30.9 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
Gibril Ndow, Yusuke Shimakawa, Damien Leith, Sulayman Bah, Rohey Bangura, Isatou Mahmoud, Lamin Bojang, Amie Ceesay, Sainabou Drammeh, Queen Bola-Lawal, Gabriel Lambert, Perrine Hardy, Patrick Ingiliz, Yazan Haddadin, Erwan Vo-Quang, Stéphane Chevaliez, Gavin Cloherty, Sheikh Omar Bittaye, Gora Lo, Coumba Toure-Kane, Maud Lemoine
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引用次数: 0

摘要

背景将抗病毒治疗扩大到根据现行国际标准不符合接受治疗条件的慢性乙型肝炎病毒(HBV)感染者的讨论越来越多。支持这种方法的证据很少,尤其是在非洲。我们旨在通过分析冈比亚未经治疗且确诊时不符合抗病毒治疗条件的慢性乙型肝炎患者的临床结果来填补这一知识空白。方法2011年12月7日至2014年1月24日期间,我们在冈比亚开展了前瞻性PROLIFICA队列研究。经过大规模社区 HBV 筛查、班珠尔 Edward Francis Small 教学医院血库 HBV 筛查以及在两个农村(Keneba 和 Manduar)通过历史性人群 HBsAg 血清调查对 HBsAg 阳性者进行前瞻性随访,我们招募了 16 岁或以上的慢性乙型肝炎参与者。参与者接受了 HBV 血清学和其他实验室检测、空腹纤维扫描和腹部超声波检查。2011年12月7日至2021年8月17日期间收集了生存数据。在 2018 年 10 月 9 日至 2021 年 8 月 17 日期间,我们邀请 2011-14 年队列中所有 HBsAg 阳性的参与者进行重新评估。在本次分析中,我们纳入了 HBsAg 阳性者,并排除了所有根据 2012 年欧洲肝脏研究协会(EASL)标准在基线时符合治疗条件的参与者,以及无论是否符合治疗条件均接受治疗的参与者。主要结果是全因死亡率,对所有有随访数据的符合治疗条件和未接受治疗的参与者进行评估。次要结局是疾病进展,分析对象是接受过重新评估的患者,疾病进展的定义是:根据2017年EASL标准,符合抗病毒治疗条件;肝纤维化至少增加一个阶段;或临床诊断为肝功能失代偿或肝细胞癌。在这 943 人中,58 人(6%)在基线时符合 2012 EASL 治疗资格标准,35 人(4%)不符合治疗资格但接受了抗病毒治疗,44 人(5%)随即失去了随访机会。因此,对806名(85%)参与者进行了主要结果分析(486名[60%]为男性,320名[40%]为女性)。经过 6-11 年(IQR 5-34-6-80)的中位数随访,708 名(88%)参与者在最后一次监测时确认存活,71 名(9%)失去随访并被剔除,27 名(3%)死亡,全因死亡率为每 10 万人年 582 例(95% CI 399-849)。在死亡的 27 人中,有 5 人(19%)死于肝脏相关疾病。在确认存活的 708 名参与者中,有 544 人(77%)接受了随访,并接受了次要结果评估。36名参与者(7%)出现了疾病进展:5人(1%)根据EASL 2017标准新近符合抗病毒治疗条件,但没有出现肝纤维化进展;18人(3%)仅出现肝纤维化进展;13人(2%)出现肝纤维化进展,并新近符合治疗标准;没有人出现肝功能失代偿或发展为肝细胞癌。在对性别和年龄进行调整后的多变量分析中,与基线HBV DNA为2000 IU/mL或更低的参考值相比,只有基线HBV DNA为20000 IU/mL或更高的参考值与肝病进展显著相关(几率比5-39,95% CI 1-37-21-23)。在这一患者亚群中扩大抗病毒治疗的临床益处仍不确定。资金来源欧盟委员会、英国医学研究理事会研究与创新部和吉利德科学公司。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Clinical outcomes of untreated adults living with chronic hepatitis B in The Gambia: an analysis of data from the prospective PROLIFICA cohort study

Background

Expanding antiviral therapy to people with chronic hepatitis B virus (HBV) infection who are ineligible to receive treatment under current international criteria has been increasingly debated. Evidence to support this approach is scarce, especially in Africa. We aimed to address this knowledge gap by analysing the clinical outcomes of people with chronic hepatitis B in The Gambia who were untreated and ineligible for antiviral therapy at diagnosis.

Methods

Between Dec 7, 2011, and Jan 24, 2014, we implemented the prospective PROLIFICA cohort study in The Gambia. Participants with chronic hepatitis B aged 16 years or older were recruited after large-scale, community-based HBV screening; blood bank-based HBV screening in Edward Francis Small Teaching Hospital, Banjul; and prospective follow-up of HBsAg-positive individuals via historical, population-based HBsAg serosurveys in two rural villages (Keneba and Manduar). Participants underwent HBV serology and other laboratory tests, fasting FibroScan, and abdominal ultrasound. Survival data were collected between Dec 7, 2011, and Aug 17, 2021. Between Oct 9, 2018, and Aug 17, 2021, all HBsAg-positive participants enrolled in the 2011–14 cohort were invited for a reassessment. For this analysis, we included HBsAg-positive people and excluded all participants who were eligible for treatment according to the 2012 European Association for the Study of the Liver (EASL) criteria at baseline and those who were treated irrespective of treatment eligibility. The primary outcome was all-cause mortality, assessed in all treatment-ineligible and treatment-naive participants with follow-up data. The secondary outcome, analysed in those who were reassessed, was disease progression, defined as becoming eligible for antivirals per 2017 EASL criteria; having an increase in liver fibrosis of at least one stage; or having a clinical diagnosis of hepatic decompensation or hepatocellular carcinoma.

Findings

943 HBsAg-positive people with chronic hepatitis B were recruited to the PROLIFICA study. Of these 943, 58 (6%) fulfilled 2012 EASL treatment eligibility criteria at baseline, 35 (4%) were ineligible for treatment but received antiviral therapy, and 44 (5%) were immediately lost to follow-up. Thus, 806 (85%) participants were analysed for the primary outcome (486 [60%] were male and 320 [40%] were female). After a median follow-up of 6·11 years (IQR 5·34–6·80), 708 (88%) participants were confirmed to be alive at last surveillance, 71 (9%) were lost to follow-up and were censored, and 27 (3%) died, giving an all-cause mortality rate of 582 per 100 000 person-years (95% CI 399–849). Of the 27 people who died, five (19%) had liver-related deaths. Of 708 participants confirmed to be alive, 544 (77%) attended follow-up and were assessed for the secondary outcome. Disease progression occurred in 36 (7%) participants: five (1%) became newly eligible for antiviral therapy per EASL 2017 criteria without liver fibrosis progression; 18 (3%) had liver fibrosis progression alone; 13 (2%) had liver fibrosis progression and newly fulfilled the treatment criteria; and none had hepatic decompensation or developed hepatocellular carcinoma. In multivariable analysis adjusted for sex and age, only a baseline HBV DNA of 20 000 IU/mL or more, compared with the baseline HBV DNA of 2000 IU/mL or lower as the reference, was significantly associated with liver disease progression (odds ratio 5·39, 95% CI 1·37–21·23).

Interpretation

Among people with chronic hepatitis B who were ineligible for antiviral therapy in The Gambia, all-cause mortality and liver disease progression were low. The clinical benefit of expanding antiviral therapy in this subgroup of patients remains uncertain.

Funding

European Commission, Medical Research Council UK Research and Innovation, and Gilead Sciences.
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来源期刊
CiteScore
50.30
自引率
1.10%
发文量
0
期刊介绍: The Lancet Gastroenterology & Hepatology is an authoritative forum for key opinion leaders across medicine, government, and health systems to influence clinical practice, explore global policy, and inform constructive, positive change worldwide. The Lancet Gastroenterology & Hepatology publishes papers that reflect the rich variety of ongoing clinical research in these fields, especially in the areas of inflammatory bowel diseases, NAFLD and NASH, functional gastrointestinal disorders, digestive cancers, and viral hepatitis.
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