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早幼粒细胞白血病蛋白(PML)异构体 II 和 V 的 C 端区域对 PML 核体形成的贡献。

Contribution of the C-terminal regions of promyelocytic leukemia protein (PML) isoforms II and V to PML nuclear body formation.

机构信息

State Key Laboratory of Agrobiotechnology, China Agricultural University, Beijing 100193, China.

出版信息

J Biol Chem. 2012 Aug 31;287(36):30729-42. doi: 10.1074/jbc.M112.374769. Epub 2012 Jul 7.

DOI:10.1074/jbc.M112.374769
PMID:22773875
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3436317/
Abstract

Promyelocytic leukemia protein (PML) nuclear bodies are dynamic and heterogeneous nuclear protein complexes implicated in various important functions, most notably tumor suppression. PML is the structural component of PML nuclear bodies and has several nuclear splice isoforms that share a common N-terminal region but differ in their C termini. Previous studies have suggested that the coiled-coil motif within the N-terminal region is sufficient for PML nuclear body formation by mediating homo/multi-dimerization of PML molecules. However, it has not been investigated whether any of the C-terminal variants of PML may contribute to PML body assembly. Here we report that the unique C-terminal domains of PML-II and PML-V can target to PML-NBs independent of their N-terminal region. Strikingly, both domains can form nuclear bodies in the absence of endogenous PML. The C-terminal domain of PML-II interacts transiently with unknown binding sites at PML nuclear bodies, whereas the C-terminal domain of PML-V exhibits hyperstable binding to PML bodies via homo-dimerization. This strong interaction is mediated by a putative α-helix in the C terminus of PML-V. Moreover, nuclear bodies assembled from the C-terminal domain of PML-V also recruit additional PML body components, including Daxx and Sp100. These observations establish the C-terminal domain of PML-V as an additional important contributor to the assembly mechanism(s) of PML bodies.

摘要

早幼粒细胞白血病蛋白 (PML) 核小体是动态的和异质的核蛋白复合物,涉及多种重要功能,尤其是肿瘤抑制。PML 是 PML 核小体的结构成分,具有几个核剪接异构体,它们共享一个共同的 N 端区域,但在 C 端不同。先前的研究表明,N 端区域内的卷曲螺旋基序足以通过介导 PML 分子的同/多二聚化来形成 PML 核小体。然而,尚未研究 PML 的任何 C 末端变体是否可能有助于 PML 体的组装。在这里,我们报告 PML-II 和 PML-V 的独特 C 末端结构域可以独立于其 N 末端结构域靶向 PML-NBs。引人注目的是,这两个结构域都可以在没有内源性 PML 的情况下形成核小体。PML-II 的 C 末端结构域与 PML 核小体上的未知结合位点短暂相互作用,而 PML-V 的 C 末端结构域通过同源二聚化与 PML 体表现出超稳定的结合。这种强相互作用是由 PML-V 的 C 末端的一个假定的α-螺旋介导的。此外,由 PML-V 的 C 末端结构域组装的核小体还招募了其他 PML 体成分,包括 Daxx 和 Sp100。这些观察结果确立了 PML-V 的 C 末端结构域是 PML 体组装机制的另一个重要贡献者。

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本文引用的文献

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De novo assembly of a PML nuclear subcompartment occurs through multiple pathways and induces telomere elongation.通过多种途径进行 PML 核亚区的从头组装,并诱导端粒延长。
J Cell Sci. 2011 Nov 1;124(Pt 21):3603-18. doi: 10.1242/jcs.084681.
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Functional connection between Rad51 and PML in homology-directed repair.Rad51 与 PML 在同源定向修复中的功能连接。
PLoS One. 2011;6(10):e25814. doi: 10.1371/journal.pone.0025814. Epub 2011 Oct 5.
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The herpesvirus associated ubiquitin specific protease, USP7, is a negative regulator of PML proteins and PML nuclear bodies.疱疹病毒相关泛素特异性蛋白酶 USP7 是 PML 蛋白和 PML 核体的负调节剂。
PLoS One. 2011 Jan 31;6(1):e16598. doi: 10.1371/journal.pone.0016598.
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PML nuclear bodies.多系统萎缩小体神经元包涵体。
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Three-dimensional organization of promyelocytic leukemia nuclear bodies.早幼粒细胞白血病核体的三维结构。
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