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Potential Therapeutic Agents for Feline Calicivirus Infection

机译:猫驯型患者感染的潜在治疗剂

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摘要

Feline calicivirus (FCV) is a major cause of upper respiratory tract disease in cats, with widespread distribution in the feline population. Recently, virulent systemic diseases caused by FCV infection has been associated with mortality rates up to 50%. Currently, there are no direct-acting antivirals approved for the treatment of FCV infection. Here, we tested 15 compounds from different antiviral classes against FCV using in vitro protein and cell culture assays. After the expression of FCV protease-polymerase protein, we established two in vitro assays to assess the inhibitory activity of compounds directly against the FCV protease or polymerase. Using this recombinant enzyme, we identified quercetagetin and PPNDS as inhibitors of FCV polymerase activity (IC 50 values of 2.8 μM and 2.7 μM, respectively). We also demonstrate the inhibition of FCV protease activity by GC376 (IC 50 of 18 μM). Using cell culture assays, PPNDS, quercetagetin and GC376 did not display antivirals effects, however, we identified nitazoxanide and 2′-C-methylcytidine (2CMC) as potent inhibitors of FCV replication, with EC 50 values in the low micromolar range (0.6 μM and 2.5 μM, respectively). In conclusion, we established two in vitro assays that will accelerate the research for FCV antivirals and can be used for the high-throughput screening of direct-acting antivirals.
机译:猫椰科(FCV)是猫的上呼吸道疾病的主要原因,猫养殖人口广泛分布。最近,由FCV感染引起的毒性全身疾病与死亡率有关,死亡率高达50%。目前,没有批准用于治疗FCV感染的直接抗病毒率。这里,我们使用体外蛋白质和细胞培养测定来测试来自不同抗病毒类的来自不同抗病毒类的化合物。在表达FCV蛋白酶 - 聚合酶蛋白质之后,我们建立了两种体外测定,以评估直接对FCV蛋白酶或聚合酶的化合物的抑制活性。使用该重组酶,我们将槲皮素和PPND鉴定为FCV聚合酶活性的抑制剂(分别为2.8μm的IC 50值和2.7μm)。我们还证明了GC376(IC 50为18μm)的FCV蛋白酶活性的抑制。使用细胞培养测定,PPNDS,槲皮素和GC376没有显示抗病毒效应,然而,我们将硝唑烷基纳和2'-C-甲基胞苷(2CMC)作为FCV复制的有效抑制剂,EC 50值(0.6μm)分别为2.5μm)。总之,我们建立了两种体外测定,将加速FCV抗病毒研究的研究,可用于直接作用抗病毒的高通量筛选。

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