肝炎病毒 A(HAV)的药物筛选:烟酰胺抑制 c-Jun 表达和 HAV 复制。
Drug Screening for Hepatitis A Virus (HAV): Nicotinamide Inhibits c-Jun Expression and HAV Replication.
机构信息
Division of Gastroenterology and Hepatology, Department of Medicine, Nihon University School of Medicine, Tokyo, Japan.
Division of Virology, Department of Infection and Immunity, Jichi Medical University School of Medicine, Shimotsuke, Tochigi, Japan.
出版信息
J Virol. 2023 Feb 28;97(2):e0198722. doi: 10.1128/jvi.01987-22. Epub 2023 Feb 2.
Hepatitis A virus (HAV) infection often causes acute hepatitis, which results in a case fatality rate of 0.2% and fulminant hepatitis in 0.5% of cases. However, no specific potent anti-HAV drug is available on the market to date. In the present study, we focused on inhibition of HAV internal ribosomal entry site (IRES)-mediated translation and investigated novel therapeutic drugs through drug repurposing by screening for inhibitors of HAV IRES-mediated translation and cell viability using a reporter assay and cell viability assay, respectively. The initial screening of 1,158 drugs resulted in 77 candidate drugs. Among them, nicotinamide significantly inhibited HAV HA11-1299 genotype IIIA replication in Huh7 cells. This promising drug also inhibited HAV HM175 genotype IB subgenomic replicon and HAV HA11-1299 genotype IIIA replication in a dose-dependent manner. In the present study, we found that nicotinamide inhibited the activation of activator protein 1 (AP-1) and that knockdown of c-Jun, which is one of the components of AP-1, inhibited HAV HM175 genotype IB IRES-mediated translation and HAV HA11-1299 genotype IIIA and HAV HM175 genotype IB replication. Taken together, the results showed that nicotinamide inhibited c-Jun, resulting in the suppression of HAV IRES-mediated translation and HAV replication, and therefore, it could be useful for the treatment of HAV infection. Drug screening methods targeting HAV IRES-mediated translation with reporter assays are attractive and useful for drug repurposing. Nicotinamide (vitamin B3, niacin) has been shown to effectively inhibit HAV replication. Transcription complex activator protein 1 (AP-1) plays an important role in the transcriptional regulation of cellular immunity or viral replication. The results of this study provide evidence that AP-1 is involved in HAV replication and plays a role in the HAV life cycle. In addition, nicotinamide was shown to suppress HAV replication partly by inhibiting AP-1 activity and HAV IRES-mediated translation. Nicotinamide may be useful for the control of acute HAV infection by inhibiting cellular AP-1 activity during HAV infection processes.
甲型肝炎病毒(HAV)感染常导致急性肝炎,其病死率为 0.2%,暴发性肝炎为 0.5%。然而,目前市场上尚无特异性强效抗 HAV 药物。本研究通过筛选 HAV IRES 介导的翻译抑制剂和细胞活力抑制剂,关注 HAV IRES 介导的翻译抑制,并通过报告基因检测和细胞活力检测分别进行药物再利用研究。对 1158 种药物进行初步筛选,得到 77 种候选药物。其中,烟酰胺显著抑制了 Huh7 细胞中 HAV HA11-1299 基因型 IIIA 的复制。这种有前景的药物还能以剂量依赖的方式抑制 HAV HM175 基因型 IB 亚基因组复制子和 HAV HA11-1299 基因型 IIIA 的复制。在本研究中,我们发现烟酰胺抑制激活蛋白 1(AP-1)的激活,而 c-Jun 的敲低(AP-1 的一个组成部分)抑制了 HAV HM175 基因型 IB IRES 介导的翻译以及 HAV HA11-1299 基因型 IIIA 和 HAV HM175 基因型 IB 的复制。综上所述,结果表明烟酰胺抑制了 c-Jun,从而抑制了 HAV IRES 介导的翻译和 HAV 复制,因此,它可能对 HAV 感染的治疗有用。用报告基因检测法筛选靶向 HAV IRES 介导的翻译的药物具有吸引力,且对药物再利用有用。烟酰胺(维生素 B3,烟酸)已被证实能有效抑制 HAV 的复制。转录复合物激活蛋白 1(AP-1)在细胞免疫或病毒复制的转录调控中发挥重要作用。本研究结果提供了证据,证明 AP-1 参与了 HAV 的复制,并在 HAV 的生命周期中发挥了作用。此外,烟酰胺通过抑制 AP-1 活性和 HAV IRES 介导的翻译,部分抑制 HAV 的复制。烟酰胺通过抑制 HAV 感染过程中细胞 AP-1 的活性,可能有助于控制急性 HAV 感染。
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