微管蛋白聚合抑制剂(SRI-32007)抑制HBV核心启动子。

IF 1.1 Q4 VIROLOGY
Advances in Virology Pub Date : 2020-10-14 eCollection Date: 2020-01-01 DOI:10.1155/2020/8844061
Raj Kalkeri, Junzhong Peng, Chunsheng Huang, Zhaohui Cai, Roger G Ptak, Mark J Suto
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引用次数: 5

摘要

全球约有2.57亿慢性乙型肝炎病毒(HBV)感染者面临发展为肝细胞癌(HCC)的风险。然而,尽管有有效的核苷/潮汐抑制剂,目前还没有治愈慢性HBV感染的治疗方法。为了确定潜在的新型抗病毒分子,一组先前在临床研究中评估过的化合物对12种不同的病毒进行了测试。在所测试的化合物中,SRI-32007 (CYT997)在HepG2.2.2.15细胞病毒产率实验中显示出抗病毒活性,50%有效浓度(EC50)和选择性指数(SI)分别为60.1 nM和7.2 nM。在分泌HBe抗原终点(EC50 40 nM和SI 250)的huh7细胞中,进一步证实了SRI-32007对HBV基因型B的抗HBV活性。为了确定SRI-32007对HBV生命周期的抑制阶段,在HepG2-NTCP细胞为基础的HBV感染实验中进行了添加时间实验。结果表明,即使在感染后72小时(72小时)添加SRI-32007也能保持抗hbv活性。另外的作用机制研究表明,SRI-32007对HBV核心启动子活性的有效抑制,EC50为40 nM, SI >250。本研究通过抑制HBV核心启动子活性证明了一种重组化合物SRI-32007的抗HBV活性。需要在HBV动物模型中进一步评估SRI-32007,以确认其体内活性。我们的实验说明了重新定位策略的效用,以确定新的抗病毒化学线索。HBV核心启动子抑制剂(如SRI-32007)可能有助于开发对抗HBV感染的新治疗策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

HBV Core Promoter Inhibition by Tubulin Polymerization Inhibitor (SRI-32007).

HBV Core Promoter Inhibition by Tubulin Polymerization Inhibitor (SRI-32007).

HBV Core Promoter Inhibition by Tubulin Polymerization Inhibitor (SRI-32007).

HBV Core Promoter Inhibition by Tubulin Polymerization Inhibitor (SRI-32007).

Approximately 257 million people chronically infected with hepatitis B virus (HBV) worldwide are at risk of developing hepatocellular carcinoma (HCC). However, despite the availability of potent nucleoside/tide inhibitors, currently there are no curative therapies for chronic HBV infections. To identify potential new antiviral molecules, a select group of compounds previously evaluated in clinical studies were tested against 12 different viruses. Amongst the compounds tested, SRI-32007 (CYT997) demonstrated antiviral activity against HBV (genotype D) in HepG2.2.2.15 cell-based virus yield assay with 50% effective concentration (EC50) and selectivity index (SI) of 60.1 nM and 7.2, respectively. Anti-HBV activity of SRI-32007 was further confirmed against HBV genotype B in huh7 cells with secreted HBe antigen endpoint (EC50 40 nM and SI 250). To determine the stage of HBV life cycle inhibited by SRI-32007, time of addition experiment was conducted in HepG2-NTCP cell-based HBV infectious assay. Results indicated that SRI-32007 retained anti-HBV activity even when added 72 hours postinfection (72 h). Additional mechanism of action studies demonstrated potent inhibition of HBV core promoter activity by SRI-32007 with an EC50 of 40 nM and SI of >250. This study demonstrates anti-HBV activity of a repurposed compound SRI-32007 through inhibition of HBV core promoter activity. Further evaluation of SRI-32007 in HBV animal models is needed to confirm its activity in vivo. Our experiments illustrate the utility of repurposing strategy to identify novel antiviral chemical leads. HBV core promoter inhibitors such as SRI-32007 might enable the development of novel therapeutic strategies to combat HBV infections.

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来源期刊
CiteScore
2.30
自引率
0.00%
发文量
23
审稿时长
22 weeks
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