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In vitro characterization of baloxavir acid, a first-in-class cap-dependent endonuclease inhibitor of the influenza virus polymerase PA subunit

机译:鲍拉洛唑酸的体外表征,流感病毒聚合酶PA亚基的一类阶层依赖性内切核酸酶抑制剂

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摘要

Cap-dependent endonuclease (CEN) resides in the PA subunit of the influenza virus and mediates the critical "cap-snatching" step of viral RNA transcription, which is considered to be a promising anti-influenza target. Here, we describe in vitro characterization of a novel CEN inhibitor, baloxavir acid (BXA), the active form of baloxavir marboxil (BXM). BXA inhibits viral RNA transcription via selective inhibition of CEN activity in enzymatic assays, and inhibits viral replication in infected cells without cytotoxicity in cytopathic effect assays. The antiviral activity of BXA is also confirmed in yield reduction assays with seasonal type A and B viruses, including neuraminidase inhibitor-resistant strains. Furthermore, BXA shows broad potency against various subtypes of influenza A viruses (H1N2, H5N1, H5N2, H5N6, H7N9 and H9N2). Additionally, serial passages of the viruses in the presence of BXA result in isolation of PA/I38T variants with reduced BXA susceptibility. Phenotypic and genotypic analyses with reverse genetics demonstrate the mechanism of BXA action via CEN inhibition in infected cells. These results reveal the in vitro characteristics of BXA and support clinical use of BXM to treat influenza.
机译:依赖性内切核酸酶(CEN)存在于流感病毒的PA亚基中,并介导病毒RNA转录的关键“帽抢”步骤,这被认为是有前途的抗流感靶标。在此,我们描述了一种新型CEN抑制剂,Baboxavir酸(BXA)的体外表征,鲍洛拉昔尔·莫博(BXM)的活性形式。 BXA通过选择性抑制酶活性的CEN活性抑制病毒RNA转录,并抑制感染细胞中的病毒复制,没有细胞毒性在细胞病变测定中。 BXA的抗病毒活性也证实了季节性A型和B病毒的屈服还原测定,包括神经氨酸酶抑制剂抗性菌株。此外,BXA对流感病毒的各种亚型(H1N2,H5N1,H5N2,H5N6,H7N9和H9N2)表示广泛的效力。另外,病毒在BXA存在下的串行通道导致具有降低的BXA易感性的PA / I38T变体。具有逆向遗传学的表型和基因型分析证明了通过CEN抑制在感染细胞中的BXA作用的机制。这些结果揭示了BXA的体外特征,并支持BXM治疗流感的临床应用。

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