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发表于 2017-6-25 16:00 |只看该作者 |倒序浏览 |打印

    J Virol. 2017 Jun 21. pii: JVI.00539-17. doi: 10.1128/JVI.00539-17. [Epub ahead of print]
    Identification of Intermediate in Hepatitis B Virus CCC DNA Formation and Sensitive and Selective CCC DNA Detection.Luo J1, Cui X1, Gao L2, Hu J3.
    Author information
    1Department of Microbiology and Immunology, The Pennsylvania State University College of Medicine, Hershey, Pennsylvania 17033, USA.2Roche Pharma Research and Early Development, Roche Innovation Center Shanghai, Shanghai 201203, China.3Department of Microbiology and Immunology, The Pennsylvania State University College of Medicine, Hershey, Pennsylvania 17033, USA [email protected].

    AbstractThe hepatitis B virus (HBV) covalently closed circular (CCC) DNA functions as the only viral template capable of coding for all the viral RNA species and is thus essential to initiate and sustain viral replication. CCC DNA is converted, in a multi-step and ill-understood process, from a relaxed circular (RC) DNA, in which neither of the two DNA strands is covalently closed. To detect putative intermediates during RC to CCC DNA conversion, two 3' exonucleases Exo I and Exo III, in combination were used to degrade all DNA strands with a free 3' end, which would nevertheless preserve closed circular DNA, either single-stranded (SS) or double-stranded (DS). Indeed, a RC DNA species with a covalently closed minus strand but an open plus strand (closed minus-strand RC DNA or cM-RC DNA) was detected by this approach. Further analyses indicated that at least some of the plus strands in such a putative intermediate likely still retained the RNA primer that is attached to the 5' end of the plus strand in RC DNA, suggesting that minus strand closing can occur before plus strand processing. Furthermore, the same nuclease treatment proved to be useful for sensitive and specific detection of CCC DNA by removing all DNA species other than closed circular DNA. Application of these and similar approaches may allow the identification of additional intermediates during CCC DNA formation and facilitate specific and sensitive detection of CCC DNA, which should help elucidate the pathways of CCC DNA formation and factors involved.IMPORTANCE The hepatitis B virus (HBV) covalently closed circular (CCC) DNA is the molecular basis of viral persistence, by serving as the viral transcriptional template. CCC DNA is converted, in a multi-step and ill-understood process, from a relaxed circular (RC) DNA. Little is currently understood about the pathways or factors involved in CCC DNA formation. We have now detected a likely intermediate during the conversion of RC to CCC DNA, thus providing important clues to the pathways of CCC DNA formation. Furthermore, the same experimental approach that led to the detection of the intermediate could also facilitate specific and sensitive detection of CCC DNA, which has remained challenging. This and similar approaches will help identify additional intermediates during CCC DNA formation and elucidate the pathways and factors involved.

    Copyright © 2017 American Society for Microbiology.



    PMID:28637752DOI:10.1128/JVI.00539-17



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才高八斗

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发表于 2017-6-25 16:00 |只看该作者
J Virol。 2017年6月21日。pii:JVI.00539-17。 doi:10.1128 / JVI.00539-17。 [提前印刷]
鉴定乙型肝炎病毒CCC DNA形成和敏感性和选择性CCC DNA检测中间体。
罗杰1,崔X1,高二,胡J3。
作者信息

1
    美国宾夕法尼亚州立大学医学院微生物和免疫学系,宾夕法尼亚州赫尔西17033,美国。
2
    罗氏制药研究与早期发展,罗氏创新中心上海,上海201203。
3
    美国宾夕法尼亚州立大学医学院微生物与免疫学系,宾夕法尼亚州赫尔西17033,[email protected]

抽象

乙型肝炎病毒(HBV)共价闭环(CCC)DNA功能作为唯一能够编码所有病毒RNA物种的病毒模板,因此启动和维持病毒复制是必不可少的。 CCC DNA在多步骤和不了解的过程中从松弛的圆形(RC)DNA转化,其中两条DNA链都不是共价闭合的。为了在RC到CCC DNA转化过程中检测推定的中间体,将两个3'外切核酸酶Exo I和Exo III组合用于以游离的3'末端降解所有DNA链,其将保持闭合的环状DNA,单链( SS)或双链(DS)。实际上,通过这种方法检测到具有共价闭合负链但是开放正链(封闭负链RC DNA或cM-RC DNA)的RC DNA物种。进一步的分析表明,这种推定的中间体中的至少一些正链可能仍保留连接到RC DNA中的正链的5'末端的RNA引物,表明负链闭合可以在正链加工之前发生。此外,相同的核酸酶处理被证明可用于通过除去除闭环的DNA以外的所有DNA物质来敏感和特异性检测CCC DNA。这些和类似方法的应用可以允许在CCC DNA形成期间鉴定其他中间体,并促进CCC DNA的特异性和灵敏检测,这有助于阐明CCC DNA形成的途径和所涉及的因素.IMPORTANCE共价乙型肝炎病毒(HBV)闭环(CCC)DNA是病毒持久性的分子基础,通过作为病毒转录模板。 CCC DNA在多步骤和不了解的过程中由轻松的圆形(RC)DNA转化。目前对于CCC DNA形成所涉及的途径或因素目前尚不清楚。我们现在已经检测到在转化为CCC DNA期间可能的中间体,从而为CCC DNA形成途径提供了重要的线索。此外,导致中间体检测的相同实验方法也可以促进对CCC DNA的特异性和灵敏检测,这仍然是具有挑战性的。这种和类似的方法将有助于在CCC DNA形成过程中鉴定其他中间体,并阐明所涉及的途径和因素。

版权所有©2017美国微生物学会。

结论:
    28637752
DOI:
    10.1128 / JVI.00539-17
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