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衔接蛋白 ARA55 和核激酶 HIPK1 协助 c-Myb 将 p300 募集到染色质上。

The adaptor protein ARA55 and the nuclear kinase HIPK1 assist c-Myb in recruiting p300 to chromatin.

机构信息

Department of Biosciences, University of Oslo, P.O. Box 1066 Blindern, N-0316 Oslo, Norway.

出版信息

Biochim Biophys Acta Gene Regul Mech. 2017 Jul;1860(7):751-760. doi: 10.1016/j.bbagrm.2017.05.001. Epub 2017 May 8.

Abstract

LIM-domain proteins, containing multiple cysteine-rich zinc finger-like motifs, have been shown to play diverse roles in several cellular processes. A common theme is that they mediate important protein-protein interactions that are key to their function. Androgen receptor-associated protein 55 (ARA55) belongs to this family of bridging proteins containing four C-terminal LIM domains. It has a dual role with functions both at focal adhesions and in the nucleus, apparently shuttling between the two compartments. In the present work, we have expanded our understanding of its nuclear functions by showing that it interacts with three nuclear regulators not previously linked to ARA55. We first identified ARA55 as a novel interaction partner of the nuclear kinase HIPK1 and found that ARA55, like HIPK1, also interacts with the transcription factor c-Myb. In search of a function for these associations, we observed that the coactivator p300 not only binds to c-Myb, but to ARA55 as well. When combined, c-Myb, p300, HIPK1 and ARA55 caused strong synergistic activation of a chromatinized reporter gene. In parallel, all partners, including p300, were efficiently recruited to chromatin at the c-Myb-bound promoter. Consistent with this cooperation, we found that c-Myb and ARA55 share a common set of target genes in an osteosarcoma cellular context. We propose that ARA55 and HIPK1 assist c-Myb in recruiting the coactivator and acetyltransferase p300 to chromatin.

摘要

LIM 结构域蛋白富含多个富含半胱氨酸的锌指样结构域,已被证明在多种细胞过程中发挥多种作用。一个共同的主题是,它们介导重要的蛋白质-蛋白质相互作用,这是它们功能的关键。雄激素受体相关蛋白 55(ARA55)属于这种桥接蛋白家族,含有四个 C 端 LIM 结构域。它具有双重作用,在黏附斑和核内都有功能,显然在这两个隔室之间穿梭。在本工作中,我们通过显示它与三个以前与 ARA55 没有联系的核调节剂相互作用,扩展了对其核功能的理解。我们首先确定 ARA55 是核激酶 HIPK1 的新的相互作用伙伴,并发现 ARA55 与 HIPK1 一样,也与转录因子 c-Myb 相互作用。为了寻找这些关联的功能,我们观察到共激活因子 p300 不仅与 c-Myb 结合,而且与 ARA55 结合。当组合在一起时,c-Myb、p300、HIPK1 和 ARA55 对染色质化报告基因产生强烈的协同激活作用。同时,所有的伙伴,包括 p300,都有效地被招募到 c-Myb 结合启动子的染色质上。与这种合作一致,我们发现 c-Myb 和 ARA55 在骨肉瘤细胞环境中共享一组共同的靶基因。我们提出 ARA55 和 HIPK1 协助 c-Myb 招募共激活因子和乙酰转移酶 p300 到染色质。

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