Tseligka Eirini D, Conzelmann Stéphanie, Cambet Yves, Schaer Tifany, Negro Francesco, Clément Sophie
Department of Pathology and Immunology, University of Geneva, Switzerland.
READS Unit, Faculty of Medicine, University of Geneva, Geneva, Switzerland.
JHEP Rep. 2022 Dec 17;5(3):100652. doi: 10.1016/j.jhepr.2022.100652. eCollection 2023 Mar.
BACKGROUND & AIMS: Chronic hepatitis delta is the most severe form of chronic viral hepatitis and is associated with faster progression towards cirrhosis, liver decompensation, and hepatocellular carcinoma. Hepatitis delta virus (HDV)'s tight dependency on hepatitis B virus and the host cell machinery for its life cycle limits the development of direct-acting antivirals. Thus, we aimed to identify compounds that could block HDV replication by targeting its antigenomic ribozyme.
We generated stable Huh7 human hepatoma cells expressing a reporter gene (Gaussia luciferase) either downstream (Gluc-2xRz) or upstream (2xRz-Gluc) of two HDV antigenomic ribozyme sequences. We performed high-throughput screening of three small molecule libraries. The secreted luciferase was measured as a readout of ribozyme inhibition upon addition of the molecules. Each plate was considered valid when the Z factor was >0.4. Specificity and toxicity evaluations were performed for the hits with a Z-score >5 and half-maximal inhibitory concentration was calculated by performing a dose-response experiment.
A dose-dependent induction of luciferase expression was detected in Gluc-2xRz-transfected cells incubated with the antisense morpholino, suggesting that the catalytic activity of the ribozyme cloned downstream of the reporter gene was efficiently inhibited. Among the 6,644 compounds screened, we identified four compounds that showed a specific inhibitory effect on the HDV antigenomic ribozyme in Gluc-2xRz cells, . three histone deacetylase inhibitors and the purine analogue 8-azaguanine. The latter also significantly decreased HDV replication (by 40%) in differentiated HepaRG cells six days post infection.
Using a novel cell culture model, we identified four small molecules active against the antigenomic HDV ribozyme. These results may provide insights into the structural requirements of molecules designed for the potent and specific inhibition of HDV replication.
Chronic hepatitis delta is the most severe form of chronic viral hepatitis and is associated with faster progression towards cirrhosis, liver decompensation, and the development of hepatocellular carcinoma. Despite the current development of several new compounds, there is still a need for efficient antiviral treatments specifically targeting hepatitis delta virus (HDV). This work describes a novel cell culture model that allows for the high-throughput screening of compounds able to inhibit HDV ribozymes. We identified four small molecules active against the antigenomic HDV ribozyme (the ribozyme involved in the early step of HDV replication), with the strongest activity shown by 8-azaguanine, a purine analogue. Our data may provide insights into the structural requirements of molecules designed to inhibit HDV.
丁型慢性肝炎是慢性病毒性肝炎最严重的形式,与肝硬化、肝失代偿及肝细胞癌的快速进展相关。丁型肝炎病毒(HDV)在其生命周期中对乙型肝炎病毒和宿主细胞机制的紧密依赖性限制了直接作用抗病毒药物的研发。因此,我们旨在鉴定能够通过靶向其反基因组核酶来阻断HDV复制的化合物。
我们构建了稳定表达报告基因(高斯荧光素酶)的Huh7人肝癌细胞系,报告基因分别位于两个HDV反基因组核酶序列的下游(Gluc-2xRz)或上游(2xRz-Gluc)。我们对三个小分子文库进行了高通量筛选。加入化合物后,检测分泌的荧光素酶以读出核酶抑制情况。当Z因子>0.4时,每块平板被认为有效。对Z分数>5的命中化合物进行特异性和毒性评估,并通过剂量反应实验计算半数最大抑制浓度。
在用反义吗啉代寡核苷酸孵育的Gluc-2xRz转染细胞中检测到荧光素酶表达的剂量依赖性诱导,这表明克隆在报告基因下游的核酶的催化活性被有效抑制。在筛选的6644种化合物中,我们鉴定出四种对Gluc-2xRz细胞中的HDV反基因组核酶具有特异性抑制作用的化合物,即三种组蛋白去乙酰化酶抑制剂和嘌呤类似物8-氮杂鸟嘌呤。后者在感染后六天也显著降低了分化的HepaRG细胞中的HDV复制(降低40%)。
使用一种新型细胞培养模型,我们鉴定出四种对反基因组HDV核酶有活性的小分子。这些结果可能为设计用于有效和特异性抑制HDV复制的分子的结构要求提供见解。
丁型慢性肝炎是慢性病毒性肝炎最严重的形式,与肝硬化、肝失代偿及肝细胞癌的快速进展相关。尽管目前有几种新化合物正在研发,但仍需要专门针对丁型肝炎病毒(HDV)的有效抗病毒治疗。这项工作描述了一种新型细胞培养模型,可用于高通量筛选能够抑制HDV核酶的化合物。我们鉴定出四种对反基因组HDV核酶(参与HDV复制早期步骤的核酶)有活性的小分子,嘌呤类似物8-氮杂鸟嘌呤显示出最强的活性。我们的数据可能为设计用于抑制HDV的分子的结构要求提供见解。
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