Combining treatment for chronic hepatitis C with opioid agonist therapy is an effective microelimination strategy for people who inject drugs with high risk of non-adherence to direct-acting antiviral therapy

IF 3.5 4区 医学 Q2 IMMUNOLOGY
M. Schwarz , C. Schwarz , A. Schütz , C. Schwanke , E. Krabb , R. Schubert , S.-T. Liebich , D. Bauer , L. Burghart , L. Brinkmann , E. Gutic , T. Reiberger , H. Haltmayer , M. Gschwantler
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引用次数: 1

Abstract

Background & aims

Despite effective direct-acting antivirals (DAAs), hepatitis C virus (HCV) prevalence is high among people who inject drugs (PWIDs) and non-adherence to therapy remains a major obstacle towards HCV elimination in this subpopulation. To overcome this issue, we have combined ongoing opioid agonist therapy (OAT) with DAAs in a directly-observed therapy (DOT) setting.

Method

From September 2014 until January 2021 PWIDs at high risk of non-adherence to DAA therapy, who were also on OAT, were included into this microelimination project. Individuals received their OAT and DAAs under supervision of healthcare workers as DOT in a pharmacy or low-threshold facility.

Results

In total, 504 HCV RNA-positive PWIDs on OAT (387 men, 76.8%; median age: 38 years [IQR 33–45], HIV: 4.6%; hepatitis B: 1.4%) were included into this study. Two thirds reported ongoing intravenous drug use (IDU) and half of them had no permanent housing. Only 41 (8.1%) were lost to follow-up and two (0.4%) died of reasons unrelated to DAA toxicity. Overall, 90.7% of PWIDs achieved sustained virological response 12 weeks after treatment (SVR12) (95% CI: 88.1–93.2%). By excluding those lost to follow-up and hose who had died of causes unrelated to DAAs, the SVR12 rate was 99.1% (95% CI: 98.3–100.0%; modified intention-to-treat analysis). Four PWIDs (0.9%) experienced treatment failure. Over a median follow-up of 24 weeks (IQR 12–39), 27 reinfections (5.9%) were observed in individuals with the highest IDU rates (81.2%). Importantly, even though some were lost to follow-up, all completed their DAA treatment. By using DOT, adherence to DAAs was excellent with only a total of 86 missed doses (0.3% of 25,224 doses).

Conclusions

In this difficult-to-treat population of PWIDs with high rates of IDU , coupling DAA treatment to OAT in a DOT setting resulted in high SVR12 rates equivalent to conventional treatment settings in non-PWID populations.

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慢性丙型肝炎联合阿片类激动剂治疗是一种有效的微消除策略,适用于注射药物的高危人群,不坚持直接作用抗病毒治疗
背景&;目的除了有效的直接作用抗病毒药物(DAAs)外,丙型肝炎病毒(HCV)在注射药物(PWID)人群中的流行率很高,不坚持治疗仍然是该亚群消除HCV的主要障碍。为了克服这个问题,我们在直接观察治疗(DOT)环境中将正在进行的阿片类激动剂治疗(OAT)与DAAs相结合。方法从2014年9月到2021年1月,未坚持DAA治疗的高危PWID,也在接受OAT,被纳入该微黎明项目。个人在药房或低门槛设施的DOT医护人员的监督下接受OAT和DAA。结果本研究共纳入504例OAT HCV RNA阳性PWID(387名男性,76.8%;中位年龄:38岁[IQR 33-45],HIV:4.6%;乙型肝炎:1.4%)。三分之二的人报告正在进行静脉注射吸毒,其中一半人没有永久住房。只有41人(8.1%)失访,2人(0.4%)死于与DAA毒性无关的原因。总的来说,90.7%的PWID在治疗12周后获得了持续的病毒学应答(SVR12)(95%CI:88.1-93.2%)。通过排除那些因与DAAs无关的原因而失去随访和软管的患者,SVR12的发生率为99.1%(95%CI:98.3-100.0%;改良意向治疗分析)。四名PWID(0.9%)出现治疗失败。在24周的中位随访(IQR 12-39)中,在IDU发病率最高(81.2%)的个体中观察到27例(5.9%)再次感染。重要的是,尽管一些患者在随访中失败,但所有人都完成了DAA治疗。通过使用DOT,对DAA的依从性非常好,总共只有86次错过剂量(25224次剂量的0.3%)。
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来源期刊
Journal of Virus Eradication
Journal of Virus Eradication Medicine-Public Health, Environmental and Occupational Health
CiteScore
6.10
自引率
1.80%
发文量
28
审稿时长
39 weeks
期刊介绍: The Journal of Virus Eradication aims to provide a specialist, open-access forum to publish work in the rapidly developing field of virus eradication. The Journal covers all human viruses, in the context of new therapeutic strategies, as well as societal eradication of viral infections with preventive interventions. The Journal is aimed at the international community involved in the prevention and management of viral infections. It provides an academic forum for the publication of original research into viral reservoirs, viral persistence and virus eradication and ultimately development of cures. The Journal not only publishes original research, but provides an opportunity for opinions, reviews, case studies and comments on the published literature. It focusses on evidence-based medicine as the major thrust in the successful management of viral infections.The Journal encompasses virological, immunological, epidemiological, modelling, pharmacological, pre-clinical and in vitro, as well as clinical, data including but not limited to drugs, immunotherapy and gene therapy. It is an important source of information on the development of vaccine programs and preventative measures aimed at virus eradication.
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