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Antiviral chemotherapy facilitates control of poxvirus infections through inhibition of cellular signal transduction

机译:抗病毒化学疗法通过抑制细胞信号转导促进控制痘病毒感染

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摘要

The EGF-like domain of smallpox growth factor (SPGF) targets human ErbB-1, inducing tyrosine phosphorylation of certain host cellular substrates via activation of the receptor’s kinase domain and thereby facilitating viral replication. Given these findings, low molecular weight organic inhibitors of ErbB-1 kinases might function as antiviral agents against smallpox. Here we show that CI-1033 and related 4-anilinoquinazolines inhibit SPGF-induced human cellular DNA synthesis, protein tyrosine kinase activation, and c-Cbl association with ErbB-1 and resultant internalization. Infection of monkey kidney BSC-40 and VERO-E6 cells in vitro by variola strain Solaimen is blocked by CI-1033, primarily at the level of secondary viral spreading. In an in vivo lethal vaccinia virus pneumonia model, CI-1033 alone promotes survival of animals, augments systemic T cell immunity and, in conjunction with a single dose of anti-L1R intracellular mature virus particle-specific mAb, fosters virtually complete viral clearance of the lungs of infected mice by the eighth day after infection. Collectively, these findings show that chemical inhibitors of host-signaling pathways exploited by viral pathogens may represent potent antiviral therapies.
机译:天花生长因子(SPGF)的EGF样结构域靶向人ErbB-1,通过激活受体的激酶结构域诱导某些宿主细胞底物的酪氨酸磷酸化,从而促进病毒复制。鉴于这些发现,ErbB-1激酶的低分子量有机抑制剂可能充当针对天花的抗病毒药物。在这里,我们显示CI-1033和相关的4-苯胺基喹唑啉抑制SPGF诱导的人类细胞DNA合成,蛋白质酪氨酸激酶活化以及与ErbB-1和产生的内在化的c-Cbl缔合。天花菌株Solaimen在体外对猴肾BSC-40和VERO-E6细胞的感染主要受CI-1033的阻断,主要是在次级病毒传播水平。在体内致命的痘苗病毒肺炎模型中,仅CI-1033就能促进动物的存活,增强全身性T细胞免疫力,并与单剂量的抗L1R细胞内成熟病毒颗粒特异性mAb结合,实际上可以促进病毒的彻底清除。感染后第8天感染小鼠的肺。总的来说,这些发现表明,病毒病原体利用的宿主信号通路化学抑制剂可能代表了有效的抗病毒治疗。

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