爱泼斯坦-巴尔病毒EBNA-1的显性负性抑制剂
Dominant-negative inhibitors of EBNA-1 of Epstein-Barr virus.
作者信息
Kirchmaier A L, Sugden B
机构信息
McArdle Laboratory for Cancer Research, University of Wisconsin Medical School, Madison 53706, USA.
出版信息
J Virol. 1997 Mar;71(3):1766-75. doi: 10.1128/JVI.71.3.1766-1775.1997.
Abstract
Epstein-Barr virus (EBV) nuclear antigen 1 (EBNA-1) is required in trans to support replication of the EBV genome once per cell cycle via the latent origin of replication, oriP. EBNA-1 can also activate transcription on binding to the family of repeats of oriP to enhance some heterologous as well as native EBV promoters. We have made and screened derivatives of EBNA-1 for the ability to act as inhibitors of wild-type EBNA-1. These derivatives lack the linking or the retention functions of EBNA-1 and were analyzed for the residual ability to activate transcription and replication. We have identified derivatives of EBNA-1 that can inhibit up to 98% of wild-type EBNA-1's activities. We have also identified one derivative of EBNA-1 with only two of EBNA-1's three linking domains which can support transcription and replication inefficiently.
摘要
爱泼斯坦-巴尔病毒(EBV)核抗原1(EBNA-1)是反式作用所必需的,它通过潜在复制起点oriP,在每个细胞周期中支持EBV基因组复制一次。EBNA-1与oriP重复序列家族结合时还能激活转录,以增强一些异源以及EBV天然启动子的活性。我们制备并筛选了EBNA-1的衍生物,以评估其作为野生型EBNA-1抑制剂的能力。这些衍生物缺乏EBNA-1的连接或保留功能,并对其激活转录和复制的残留能力进行了分析。我们鉴定出了能抑制高达98%野生型EBNA-1活性的EBNA-1衍生物。我们还鉴定出一种EBNA-1衍生物,它仅具有EBNA-1三个连接结构域中的两个,只能低效地支持转录和复制。
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