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HBV Capsid装配调节剂,但不是核苷类似物,抑制细胞外前基因 [复制链接]

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发表于 2017-6-1 16:11 |只看该作者 |倒序浏览 |打印

    Antimicrob Agents Chemother. 2017 May 30. pii: AAC.00680-17. doi: 10.1128/AAC.00680-17. [Epub ahead of print]
    HBV Capsid Assembly Modulators, but not Nucleoside Analogs, Inhibit the Production of Extracellular Pregenomic RNA and Spliced RNA Variants.Lam AM1, Ren S2, Espiritu C2, Kelly M2, Lau V2, Zheng L2, Hartman GD2, Flores OA2, Klumpp K2.
    Author information
    1Novira Therapeutics Inc, part of the Janssen Pharmaceutical Companies, 1400 McKean Road, Spring House, PA 19477, USA [email protected].2Novira Therapeutics Inc, part of the Janssen Pharmaceutical Companies, 1400 McKean Road, Spring House, PA 19477, USA.

    AbstractThe Hepatitis B virus (HBV) core protein serves multiple essential functions in the viral life cycle and is being developed as a target for antiviral agents. Capsid assembly modulators (CAMs) are compounds that target core and misdirect capsid assembly, resulting in the suppression of HBV replication and virion production. Besides HBV DNA, circulating HBV RNA has been detected in patient serum and can be associated with treatment response. Here we studied the effect of HBV CAMs on the production of extracellular HBV RNA using infected HepaRG cells and primary human hepatocytes. Representative compounds from the sulfonamide carboxamide and heteroaryldihydropyrimidine series of CAMs were evaluated and compared to nucleos(t)ide analogs as inhibitors of the viral polymerase. Results showed that CAMs blocked extracellular HBV RNA with similar efficiencies as pgRNA encapsidation, HBV DNA replication, and Dane particles production. Nucleos(t)ide analogs inhibited viral replication and virion production, but not encapsidation or production of extracellular HBV RNA. Profiling of HBV RNA from both cultured supernatants and patient serum showed that extracellular viral RNA consisted of pgRNA and spliced pgRNA variants with internal deletion(s) but still retained the sequences at both 5' and 3' ends. Similar variants were detected in the supernatants of infected cells with and without nucleos(t)ide analog treatment. Overall, our data demonstrates that HBV CAMs represent direct antiviral agents with a differentiated profile as compared to nucleos(t)ide analogs, including the inhibition of extracellular pgRNA and spliced pgRNA.

    Copyright © 2017 Lam et al.



    PMID:28559265DOI:10.1128/AAC.00680-17



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发表于 2017-6-1 16:11 |只看该作者
抗微生物剂2017年5月30日。pii:AAC.00680-17。 doi:10.1128 / AAC.00680-17。 [提前印刷]
HBV Capsid装配调节剂,但不是核苷类似物,抑制细胞外前基因组RNA和剪接的RNA变体的产生。
Lam AM1,Ren S2,Espiritu C2,Kelly M2,Lau V2,Zheng L2,Hartman GD2,Flores OA2,Klumpp K2。
作者信息

1
    Novira Therapeutics Inc,Janssen Pharmaceutical Companies的一部分,1400 McKean Road,Spring House,PA 19477,USA [email protected]
2
    Novira Therapeutics公司,扬森制药公司的一部分,1400 McKean Road,Spring House,PA 19477,USA。

抽象

乙型肝炎病毒(HBV)核心蛋白在病毒生命周期中起着多种基本功能的作用,并被开发为抗病毒药物的靶标。衣壳装配调制剂(CAMs)是靶向核心和错误定位衣壳装配的化合物,导致HBV复制和病毒粒子产生的抑制。除了HBV DNA外,已经在患者血清中检测到循环的HBV RNA,并且可以与治疗反应相关。在这里,我们研究了HBV CAMs对使用感染的HepaRG细胞和原代人肝细胞产生细胞外HBV RNA的影响。评估来自磺酰胺羧酰胺和杂芳基二氢嘧啶系列CAM的代表性化合物,并将其与核苷(t)ide类似物作为病毒聚合酶的抑制剂进行比较。结果表明,CAMs阻断了细胞外HBV RNA,具有与pgRNA包膜,HBV DNA复制和Dane颗粒生产相似的效力。 Nucleos(t)ide类似物抑制病毒复制和病毒粒子产生,但不抑制细胞外HBV RNA的包囊或产生。从培养的上清液和患者血清中分析HBV RNA显示细胞外病毒RNA由具有内部缺失的pgRNA和剪接的pgRNA变体组成,但仍保留5'和3'末端的序列。在有或没有核苷类似物处理的感染细胞的上清液中检测到相似的变体。总体而言,我们的数据表明,HBV CAMs代表与核苷类似物相比具有差异分布特征的直接抗病毒药物,包括细胞外pgRNA和剪接的pgRNA的抑制。

版权所有©2017 Lam et al。

结论:
    28559265
DOI:
    10.1128 / AAC.00680-17

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3
发表于 2017-6-1 16:14 |只看该作者
阅读好文章,传播正能量

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4
发表于 2017-6-1 23:10 |只看该作者
只有靶向 RNA 和核衣壳 才是正确的方向。
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