首页> 美国卫生研究院文献>The Journal of General Virology >Analysis of the anti-apoptotic activity of four vaccinia virus proteins demonstrates that B13 is the most potent inhibitor in isolation and during viral infection
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Analysis of the anti-apoptotic activity of four vaccinia virus proteins demonstrates that B13 is the most potent inhibitor in isolation and during viral infection

机译:对四种痘苗病毒蛋白的抗凋亡活性的分析表明B13是分离和病毒感染期间最有效的抑制剂

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摘要

Vaccinia virus (VACV) is a large dsDNA virus encoding ~200 proteins, several of which inhibit apoptosis. Here, a comparative study of anti-apoptotic proteins N1, F1, B13 and Golgi anti-apoptotic protein (GAAP) in isolation and during viral infection is presented. VACVs strains engineered to lack each gene separately still blocked apoptosis to some degree because of functional redundancy provided by the other anti-apoptotic proteins. To overcome this redundancy, we inserted each gene separately into a VACV strain (vv811) that lacked all these anti-apoptotic proteins and that induced apoptosis efficiently during infection. Each protein was also expressed in cells using lentivirus vectors. In isolation, each VACV protein showed anti-apoptotic activity in response to specific stimuli, as measured by immunoblotting for cleaved poly(ADP ribose) polymerase-1 and caspase-3 activation. Of the proteins tested, B13 was the most potent inhibitor, blocking both intrinsic and extrinsic stimuli, whilst the activity of the other proteins was largely restricted to inhibition of intrinsic stimuli. In addition, B13 and F1 were effective blockers of apoptosis induced by vv811 infection. Finally, whilst differences in induction of apoptosis were barely detectable during infection with VACV strain Western Reserve compared with derivative viruses lacking individual anti-apoptotic genes, several of these proteins reduced activation of caspase-3 during infection by vv811 strains expressing these proteins. These results illustrated that vv811 was a useful tool to determine the role of VACV proteins during infection and that whilst all of these proteins have some anti-apoptotic activity, B13 was the most potent.
机译:牛痘病毒(VACV)是一种大型dsDNA病毒,编码约200种蛋白质,其中一些抑制凋亡。在这里,进行了抗凋亡蛋白N1,F1,B13和高尔基抗凋亡蛋白(GAAP)的分离研究以及在病毒感染过程中的比较研究。经过工程设计以分别缺少每个基因的VACVs菌株,由于其他抗凋亡蛋白提供的功能冗余,仍在一定程度上阻止了细胞凋亡。为了克服这种冗余,我们将每个基因分别插入到VACV株(vv811)中,该株缺少所有这些抗凋亡蛋白,并在感染过程中有效诱导了细胞凋亡。使用慢病毒载体还在细胞中表达每种蛋白质。孤立地,每种VACV蛋白都表现出对特定刺激的抗凋亡活性,这是通过免疫印迹法检测裂解的多聚(ADP核糖)聚合酶-1和caspase-3的活化来进行的。在测试的蛋白质中,B13是最有效的抑制剂,可阻断内在和外在刺激,而其他蛋白质的活性在很大程度上限于抑制内在刺激。此外,B13和F1是vv811感染诱导的有效凋亡抑制剂。最后,尽管与缺少单个抗凋亡基因的衍生病毒相比,在用VACV株Western Reserve感染期间几乎无法检测到诱导凋亡的差异,但这些蛋白中的一些蛋白在表达这些蛋白的vv811菌株感染期间降低了caspase-3的活化。这些结果说明,vv811是确定VACV蛋白在感染过程中的作用的有用工具,尽管所有这些蛋白均具有一定的抗凋亡活性,但B13是最有效的。

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