干扰素诱导蛋白 16:与肿瘤抑制因子 p53 相互作用的研究进展。
Interferon-inducible protein 16: insight into the interaction with tumor suppressor p53.
机构信息
Campbell Family Cancer Research Institute, Ontario Cancer Institute, University Health Network, Toronto, ON M5G 2C4, Canada.
出版信息
Structure. 2011 Mar 9;19(3):418-29. doi: 10.1016/j.str.2010.12.015.
Abstract
IFI16 is a member of the interferon-inducible HIN-200 family of nuclear proteins. It has been implicated in transcriptional regulation by modulating protein-protein interactions with p53 tumor suppressor protein and other transcription factors. However, the mechanisms of interaction remain unknown. Here, we report the crystal structures of both HIN-A and HIN-B domains of IFI16 determined at 2.0 and 2.35 Å resolution, respectively. Each HIN domain comprises a pair of tightly packed OB-fold subdomains that appear to act as a single unit. We show that both HIN domains of IFI16 are capable of enhancing p53-DNA complex formation and transcriptional activation via distinctive means. HIN-A domain binds to the basic C terminus of p53, whereas the HIN-B domain binds to the core DNA-binding region of p53. Both interactions are compatible with the DNA-bound state of p53 and together contribute to the effect of full-length IFI16 on p53-DNA complex formation and transcriptional activation.
摘要
IFI16 是干扰素诱导的 HIN-200 家族核蛋白的成员。它通过调节与 p53 肿瘤抑制蛋白和其他转录因子的蛋白-蛋白相互作用而参与转录调控。然而,其相互作用的机制尚不清楚。在这里,我们报告了 IFI16 的 HIN-A 和 HIN-B 结构域的晶体结构,分别在 2.0 和 2.35 Å 分辨率下确定。每个 HIN 结构域由一对紧密堆积的 OB 折叠亚结构域组成,它们似乎作为一个整体发挥作用。我们表明,IFI16 的两个 HIN 结构域都能够通过独特的方式增强 p53-DNA 复合物的形成和转录激活。HIN-A 结构域与 p53 的碱性 C 末端结合,而 HIN-B 结构域与 p53 的核心 DNA 结合区域结合。这两种相互作用都与 p53 的 DNA 结合状态兼容,并共同促成全长 IFI16 对 p53-DNA 复合物形成和转录激活的影响。
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