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以酵母病毒杀伤系统为基础的抗病毒药物筛选模型 被引量:1
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作者 叶燕锐 潘力 《中国抗生素杂志》 CAS CSCD 北大核心 2006年第8期449-452,500,共5页
许多病毒利用程序性-1核糖体移码作为翻译调节机制进行繁殖。程序性酵母的病毒杀伤系统由L-A病毒和M1卫星病毒组成。M1病毒编码一种分泌型毒素K1,能杀死不含病毒的酵母细胞,但有自身免疫功能。L-A通过一定频率-1移码事件进行繁殖,-1移... 许多病毒利用程序性-1核糖体移码作为翻译调节机制进行繁殖。程序性酵母的病毒杀伤系统由L-A病毒和M1卫星病毒组成。M1病毒编码一种分泌型毒素K1,能杀死不含病毒的酵母细胞,但有自身免疫功能。L-A通过一定频率-1移码事件进行繁殖,-1移码效率的改变影响L-A病毒的存活,使M1数量快速下降。因此以程序性-1核糖体移码为靶位,建立以酵母病毒杀伤系统为基础的筛选模型,在抗病毒药物的高通量筛选方面有良好的应用前景。 展开更多
关键词 酵母杀伤系统 程序性-1核糖体移码 抗病毒药物
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C19orf66 Inhibits Japanese Encephalitis Virus Replication by Targeting-1 PRF and the NS3 Protein 被引量:1
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作者 Du Yu Yundi Zhao +4 位作者 Junhui Pan Xingmiao Yang Zhenjie Liang Shengda Xie Ruibing Cao 《Virologica Sinica》 SCIE CAS CSCD 2021年第6期1443-1455,共13页
The Japanese encephalitis serogroup of the neurogenic Flavivirus has a specific feature that expresses a non-structural protein NS1'produced through a programmed-1 ribosomal frameshifting(-1 PRF).Herein,C19orf66,a... The Japanese encephalitis serogroup of the neurogenic Flavivirus has a specific feature that expresses a non-structural protein NS1'produced through a programmed-1 ribosomal frameshifting(-1 PRF).Herein,C19orf66,a novel member of interferon-stimulated gene(ISG)products,exhibited significant activity of antagonizing Japanese encephalitis virus(JEV)infection.Overexpression of C19orf66 in 293T cells significantly inhibited JEV replication,while knock-down of endogenous C19orf66 in HeLa cells and A549 cells significantly increased virus replication.Notably,C19orf66 had an inhibitory effect on frameshift production of JEV NS1'.The inhibition was more significant when C19orf66 and JEV NS1-NS2A were co-expressed in the 293T cells.Both C19orf66-209 and C19orf66-Zinc^(mut) did not significantly change the NS1'to NS1 ratio and had weaker antiviral effects than C19orf66.Similarly,C19orf66-209 and C19orf66-Zinc^(mut) had no significant effect on the expression of the JEV NS3 protein,whose expression was down-regulated by C19orf66 via the lysosome-dependent pathway.These findings suggest that C19orf66 may possess at least two different mechanisms of antagonizing JEV infection.This study identified C19orf66 as a novel interferon-stimulated gene product that can inhibit JEV replication by targeting-1 PRF and the NS3 protein.The study provides baseline information for the future development of broad-spectrum antiviral agents against JEV. 展开更多
关键词 Japanese encephalitis virus(JEV) C19orf66 programmed-1 ribosomal frameshifting(-1 PRF) NS1 NS3
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