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C4 亚基因型乙型肝炎感染的疾病进展与治疗需求:澳大利亚北领地的一项回顾性队列研究

Disease progression & treatment need in sub-genotype C4 hepatitis B infection: a retrospective cohort study in the Northern Territory, Australia.

作者信息

Martin Genevieve E, Hosking Kelly, Banz Kelly, Gargan Catherine, Stewart Geoff, Greenwood-Smith Belinda, Ramsay Penelope, Tate-Baker Jaclyn, Connors Christine, Binks Paula, McKinnon Melita, Manchikanti Prashanti, Gurruwiwi George Garambaka, Allard Nicole, Qama Ashleigh, Michaels Jessica, Vintour-Cesar Emily, Batey Robert, Marshall Catherine, Nihill Peter, Fernandes Tammy-Allyn, Fuller Karen, Tong Steven Y C, Boettiger David, Cowie Benjamin, Davis Joshua S, Bukulatjpi Sarah Mariyalawuy, Davies Jane

机构信息

Global and Tropical Health Division, Menzies School of Health Research, Charles Darwin University, Darwin, NT, Australia.

Northern Territory Health, Northern Territory, Australia.

出版信息

BMC Infect Dis. 2025 Jul 1;25(1):881. doi: 10.1186/s12879-025-11213-w.

Abstract

BACKGROUND

In the Northern Territory (NT) of Australia, First Nations people with chronic hepatitis B (CHB) are infected with a unique sub-genotype, C4, which contains mutations linked to progressive fibrosis and hepatocellular carcinoma. This cohort study aimed to investigate disease progression in C4 sub-genotype infection and estimate how many untreated individuals may benefit from antiviral therapy with broadening treatment indications.

METHODS

Included individuals were part of Hep B PAST, a co-designed program to improve the cascade of care for people living with CHB in the NT. Disease phase and cirrhotic status were determined algorithmically using clinical and laboratory data at two time points. Loss of HBV antigens was assessed longitudinally. Treatment need was assessed cross-sectionally in the cohort at study completion. Key outcomes were estimated rates of HBsAg/HBeAg loss in sub-genotype C4 infection and quantification of how many untreated individuals qualify for therapy under current Australian and expanded global treatment guidelines.

RESULTS

HBsAg and HBeAg loss occurred at a rate of 1·04 and 8·06 events/100 person-years respectively (7342·6 and 545·6 years follow up). 783 people living with CHB were included (40% female, median age 48 years). Of these, 16% had cirrhosis (an additional 6% having FibroScan > 7 kPa, meaning 22% had cirrhosis or significant fibrosis) and 25% were prescribed antivirals. Only 6·7% of untreated individuals were treatment eligible under current guidelines. Using the 2024 World Health Organisation guidelines, this increased to 50% due mostly to fibrosis and population prevalence of diabetes.

CONCLUSIONS

Despite advanced liver disease in people living with CHB in the NT, rates of antigen loss in sub-genotype C4 hepatitis B infection are similar to other genotypes. Further work is needed to understand drivers of cirrhosis and significant fibrosis in this population.

摘要

背景

在澳大利亚北领地(NT),患有慢性乙型肝炎(CHB)的原住民感染了一种独特的C4亚基因型,该亚基因型包含与进行性纤维化和肝细胞癌相关的突变。这项队列研究旨在调查C4亚基因型感染的疾病进展,并估计有多少未接受治疗的个体可能从扩大治疗指征的抗病毒治疗中获益。

方法

纳入的个体是乙肝既往治疗(Hep B PAST)项目的一部分,该项目是一个共同设计的项目,旨在改善北领地CHB患者的护理流程。使用两个时间点的临床和实验室数据,通过算法确定疾病阶段和肝硬化状态。纵向评估乙肝病毒抗原的消失情况。在研究结束时,对队列中的治疗需求进行横断面评估。主要结局是估计C4亚基因型感染中乙肝表面抗原(HBsAg)/乙肝e抗原(HBeAg)消失的发生率,以及根据当前澳大利亚和扩大后的全球治疗指南,量化有多少未接受治疗的个体符合治疗条件。

结果

HBsAg和HBeAg消失的发生率分别为1.04和8.06事件/100人年(随访7342.6和545.6人年)。纳入了783例CHB患者(40%为女性,中位年龄48岁)。其中,16%患有肝硬化(另有6%的FibroScan值>7 kPa,意味着22%患有肝硬化或显著纤维化),25%的患者接受了抗病毒治疗。根据当前指南,只有6.7%的未接受治疗的个体符合治疗条件。采用2024年世界卫生组织指南,这一比例增至50%,主要原因是纤维化和糖尿病在人群中的患病率。

结论

尽管北领地CHB患者存在晚期肝病,但C4亚基因型乙型肝炎感染的抗原消失率与其他基因型相似。需要进一步开展工作,以了解该人群中肝硬化和显著纤维化的驱动因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/399d/12219930/cc8c85c452f7/12879_2025_11213_Fig1_HTML.jpg

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