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标题: HBV转录本的治疗性关闭可促进SMC5 / 6复合体的再现并体内病毒 [打印本页]

作者: StephenW    时间: 2021-1-31 03:13     标题: HBV转录本的治疗性关闭可促进SMC5 / 6复合体的再现并体内病毒


Therapeutic shutdown of HBV transcripts promotes reappearance of the SMC5/6 complex and silencing of the viral genome in vivo

    Lena Allweiss1, Katja Giersch1, Andrea Pirosu1, http://orcid.org/0000-0003-3120-8958Tassilo Volz1,2, Robert C Muench3, Rudolf K Beran3, Stephan Urban2,4, Hassan Javanbakht3, Simon P Fletcher3, Marc Lütgehetmann2,5, http://orcid.org/0000-0002-0073-6689Maura Dandri1,2

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Abstract

Objective Silencing of the therapeutic strategies and reducing the HBV reservoir, the covalently closed circular DNA (cccDNA), have the potential to cure chronic HBV infection. We aimed to investigate the impact of small interferring RNA (siRNA) targeting all HBV transcripts or pegylated interferon-α (peg-IFNα) on the viral regulatory HBx protein and the structural maintenance of chromosome 5/6 complex (SMC5/6), a host factor suppressing cccDNA transcription. In particular, we assessed whether interventions lowering HBV transcripts can achieve and maintain silencing of cccDNA transcription in vivo.

Design HBV-infected human liver chimeric mice were treated with siRNA or peg-IFNα. Virological and host changes were analysed at the end of treatment and during the rebound phase by qualitative PCR, ELISA, immunoblotting and chromatin immunoprecipitation. RNA in situ hybridisation was combined with immunofluorescence to detect SMC6 and HBV RNAs at single cell level. The entry inhibitor myrcludex-B was used during the rebound phase to avoid new infection events.

Results Both siRNA and peg-IFNα strongly reduced all HBV markers, including HBx levels, thus enabling the reappearance of SMC5/6 in hepatocytes that achieved HBV-RNA negativisation and SMC5/6 association with the cccDNA. Only IFN reduced cccDNA loads and enhanced IFN-stimulated genes. However, the antiviral effects did not persist off treatment and SMC5/6 was again degraded. Remarkably, the blockade of viral entry that started at the end of treatment hindered renewed degradation of SMC5/6.

Conclusion These results reveal that therapeutics abrogating all HBV transcripts including HBx promote epigenetic suppression of the HBV minichromosome, whereas strategies protecting the human hepatocytes from reinfection are needed to maintain cccDNA silencing.
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http://dx.doi.org/10.1136/gutjnl-2020-322571

作者: StephenW    时间: 2021-1-31 03:14

HBV转录本的治疗性关闭可促进SMC5 / 6复合体的再现并体内病毒基因组沉默

    Lena Allweiss1,Katja Giersch1,Andrea Pirosu1,http://orcid.org/0000-0003-3120-8958Tassilo Volz1,2,Robert C Muench3,Rudolf K Beran3,Stephan Urban2.4、4,Hassan Javanbakht3,Simon P Fletcher3,MarcLütgehetmann2 ,5,http://orcid.org/0000-0002-0073-6689Maura Dandri1,2

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目的沉默治疗策略并减少HBV储库(共价闭合环状DNA(cccDNA))具有治愈慢性HBV感染的潜力。我们旨在研究针对所有HBV转录本或聚乙二醇化干扰素-α(peg-IFNα)的小干扰RNA(siRNA)对病毒调节HBx蛋白的影响以及5/6号染色体复合体(SMC5 / 6)的结构维持宿主因子抑制cccDNA转录。特别是,我们评估了降低HBV转录本的干预措施能否在体内实现和维持cccDNA转录的沉默。

用siRNA或peg-IFNα处理设计的HBV感染的人肝嵌合小鼠。在治疗结束时和反弹阶段,通过定性PCR,ELISA,免疫印迹和染色质免疫沉淀分析病毒学和宿主变化。 RNA原位杂交与免疫荧光相结合,可在单细胞水平检测SMC6和HBV RNA。在反弹阶段使用进入抑制剂myrcludex-B以避免新的感染事件。

结果siRNA和peg-IFNα都强烈降低了所有HBV标记,包括HBx水平,从而使SMC5 / 6在实现HBV-RNA阴性和SMC5 / 6与cccDNA结合的肝细胞中重新出现。只有IFN减少了cccDNA的负载并增强了IFN刺激的基因。但是,抗病毒作用并未在治疗后持续存在,SMC5 / 6再次降解。值得注意的是,在治疗结束时开始的病毒进入阻断阻止了SMC5 / 6的新降解。

结论这些结果表明,废除包括HBx在内的所有HBV转录物的疗法可促进HBV微型染色体的表观遗传学抑制,而需要保护人肝细胞免于再次感染的策略以维持cccDNA沉默。
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http://dx.doi.org/10.1136/gutjnl-2020-322571
作者: StephenW    时间: 2021-1-31 03:15

https://gut.bmj.com/content/gutj ... 020-322571.full.pdf




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