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肝胆相照论坛 论坛 学术讨论& HBV English 细胞内干扰素信号通路作为慢性乙型肝炎治疗中共价闭合环 ...
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细胞内干扰素信号通路作为慢性乙型肝炎治疗中共价闭合环 [复制链接]

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发表于 2021-4-30 15:17 |只看该作者 |倒序浏览 |打印
Intracellular interferon signalling pathways as potential regulators of covalently closed circular DNA in the treatment of chronic hepatitis B
Zhi Yi Goh  1 , Ee Chee Ren  1 , Hui Ling Ko  2
Affiliations
Affiliations

    1
    Singapore Immunology Network, Agency for Science, Technology and Research, Singapore 138648, Singapore.
    2
    Singapore Immunology Network, Agency for Science, Technology and Research, Singapore 138648, Singapore. [email protected].

    PMID: 33911462 PMCID: PMC8047536 DOI: 10.3748/wjg.v27.i14.1369

Abstract

Infection with the hepatitis B virus (HBV) is still a major global health threat as 250 million people worldwide continue to be chronically infected with the virus. While patients may be treated with nucleoside/nucleotide analogues, this only suppresses HBV titre to sub-detection levels without eliminating the persistent HBV covalently closed circular DNA (cccDNA) genome. As a result, HBV infection cannot be cured, and the virus reactivates when conditions are favorable. Interferons (IFNs) are cytokines known to induce powerful antiviral mechanisms that clear viruses from infected cells. They have been shown to induce cccDNA clearance, but their use in the treatment of HBV infection is limited as HBV-targeting immune cells are exhausted and HBV has evolved multiple mechanisms to evade and suppress IFN signalling. Thus, to fully utilize IFN-mediated intracellular mechanisms to effectively eliminate HBV, instead of direct IFN administration, novel strategies to sustain IFN-mediated anti-cccDNA and antiviral mechanisms need to be developed. This review will consolidate what is known about how IFNs act to achieve its intracellular antiviral effects and highlight the critical interferon-stimulated gene targets and effector mechanisms with potent anti-cccDNA functions. These include cccDNA degradation by APOBECs and cccDNA silencing and transcription repression by epigenetic modifications. In addition, the mechanisms that HBV employs to disrupt IFN signalling will be discussed. Drugs that have been developed or are in the pipeline for components of the IFN signalling pathway and HBV targets that detract IFN signalling mechanisms will also be identified and discussed for utility in the treatment of HBV infections. Together, these will provide useful insights into design strategies that specifically target cccDNA for the eradication of HBV.

Keywords: APOBECs; Covalently closed circular DNA; Epigenetic modification; Hepatitis B virus therapeutics; Interferons.

©The Author(s) 2021. Published by Baishideng Publishing Group Inc. All rights reserved.

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发表于 2021-4-30 15:18 |只看该作者
细胞内干扰素信号通路作为慢性乙型肝炎治疗中共价闭合环状DNA的潜在调节剂
吴志仪1,易志人1,慧玲子2
隶属关系
隶属关系

    1个
    科学技术研究局新加坡免疫学网络,新加坡138648,新加坡。
    2个
    科学技术研究局新加坡免疫学网络,新加坡138648,新加坡。 [email protected]

    PMID:33911462 PMCID:PMC8047536 DOI:10.3748 / wjg.v27.i14.1369

抽象的

乙型肝炎病毒(HBV)的感染仍然是全球主要的健康威胁,因为全球有2.5亿人继续受到该病毒的慢性感染。尽管可以使用核苷/核苷酸类似物治疗患者,但这只能将HBV滴度抑制至亚检测水平,而不会消除持久性HBV共价闭合环状DNA(cccDNA)基因组。结果,无法治愈HBV感染,并且在条件允许时病毒会重新激活。干扰素(IFN)是已知诱导强大的抗病毒机制的细胞因子,这种机制可以清除感染细胞中的病毒。已显示它们可诱导cccDNA清除,但是由于靶向HBV的免疫细胞已耗尽,并且HBV进化出多种逃避和抑制IFN信号传导的机制,因此它们在HBV感染治疗中的应用受到限制。因此,为了充分利用IFN介导的细胞内机制有效消除HBV,而不是直接施用IFN,需要开发新的策略来维持IFN介导的抗cccDNA和抗病毒机制。这篇综述将巩固有关IFN如何发挥作用以实现其细胞内抗病毒作用的已知信息,并重点介绍干扰素刺激的关键基因靶标和具有有效抗cccDNA功能的效应子机制。这些包括由APOBECs引起的cccDNA降解和通过表观遗传修饰的cccDNA沉默和转录抑制。此外,将讨论HBV破坏IFN信号传导的机制。还将确定和讨论已开发出或正在开发干扰IFN信号通路成分的药物以及削弱IFN信号传导机制的HBV靶标,以用于治疗HBV感染。在一起,这些将为特别针对cccDNA根除HBV的设计策略提供有用的见解。

关键字:APOBEC;共价封闭的环状DNA;表观遗传修饰;乙型肝炎病毒疗法;干扰素。

©2021年作者。百世登出版集团有限公司出版。保留所有权利。

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现金
62111 元 
精华
26 
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30437 
注册时间
2009-10-5 
最后登录
2022-12-28 

才高八斗

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发表于 2021-4-30 15:18 |只看该作者
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