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Recruitment of the nucleolar remodeling complex NoRC establishes ribosomal DNA silencing in chromatin.核仁重塑复合体NoRC的募集在染色质中建立核糖体DNA沉默。
Mol Cell Biol. 2004 Feb;24(4):1791-8. doi: 10.1128/MCB.24.4.1791-1798.2004.
2
The PHD finger/bromodomain of NoRC interacts with acetylated histone H4K16 and is sufficient for rDNA silencing.NoRC的PHD结构域/溴结构域与乙酰化组蛋白H4K16相互作用,并且足以实现核糖体DNA沉默。
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Epigenetic mechanism of rRNA gene silencing: temporal order of NoRC-mediated histone modification, chromatin remodeling, and DNA methylation.核糖体RNA基因沉默的表观遗传机制:NoRC介导的组蛋白修饰、染色质重塑和DNA甲基化的时间顺序。
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本文引用的文献

1
The nucleolar remodeling complex NoRC mediates heterochromatin formation and silencing of ribosomal gene transcription.核仁重塑复合体NoRC介导异染色质形成及核糖体基因转录沉默。
Nat Genet. 2002 Nov;32(3):393-6. doi: 10.1038/ng1010. Epub 2002 Oct 7.
2
The chromatin remodeling complex NoRC targets HDAC1 to the ribosomal gene promoter and represses RNA polymerase I transcription.染色质重塑复合物NoRC将HDAC1靶向核糖体基因启动子并抑制RNA聚合酶I转录。
EMBO J. 2002 Sep 2;21(17):4632-40. doi: 10.1093/emboj/cdf460.
3
NoRC--a novel member of mammalian ISWI-containing chromatin remodeling machines.NoRC——哺乳动物含ISWI染色质重塑机器的一个新成员。
EMBO J. 2001 Sep 3;20(17):4892-900. doi: 10.1093/emboj/20.17.4892.
4
Acf1, the largest subunit of CHRAC, regulates ISWI-induced nucleosome remodelling.ACF1是染色质重塑因子(CHRAC)的最大亚基,可调节ISWI诱导的核小体重塑。
EMBO J. 2001 Jul 16;20(14):3781-8. doi: 10.1093/emboj/20.14.3781.
5
Functional differences between the human ATP-dependent nucleosome remodeling proteins BRG1 and SNF2H.人类ATP依赖型核小体重塑蛋白BRG1和SNF2H之间的功能差异。
J Biol Chem. 2001 Sep 7;276(36):34270-8. doi: 10.1074/jbc.M104163200. Epub 2001 Jul 2.
6
Critical role for the histone H4 N terminus in nucleosome remodeling by ISWI.组蛋白H4 N端在ISWI介导的核小体重塑中起关键作用。
Mol Cell Biol. 2001 Feb;21(3):875-83. doi: 10.1128/MCB.21.3.875-883.2001.
7
Nucleosome movement by CHRAC and ISWI without disruption or trans-displacement of the histone octamer.染色质重塑和ATP酶(CHRAC)及模仿SWI2/SNF2的ATP酶(ISWI)介导的核小体移动,而不破坏或转位组蛋白八聚体。
Cell. 1999 Jun 25;97(7):843-52. doi: 10.1016/s0092-8674(00)80797-7.
8
ACF consists of two subunits, Acf1 and ISWI, that function cooperatively in the ATP-dependent catalysis of chromatin assembly.自组装染色质因子(ACF)由两个亚基组成,即Acf1和ISWI,它们在依赖ATP的染色质组装催化过程中协同发挥作用。
Genes Dev. 1999 Jun 15;13(12):1529-39. doi: 10.1101/gad.13.12.1529.
9
ISWI is an ATP-dependent nucleosome remodeling factor.ISWI是一种依赖ATP的核小体重塑因子。
Mol Cell. 1999 Feb;3(2):239-45. doi: 10.1016/s1097-2765(00)80314-7.
10
Structure, dynamics, and function of chromatin in vitro.体外染色质的结构、动力学及功能
Annu Rev Biophys Biomol Struct. 1998;27:285-327. doi: 10.1146/annurev.biophys.27.1.285.

核仁重塑复合体NoRC的募集在染色质中建立核糖体DNA沉默。

Recruitment of the nucleolar remodeling complex NoRC establishes ribosomal DNA silencing in chromatin.

作者信息

Strohner Ralf, Németh Attila, Nightingale Karl P, Grummt Ingrid, Becker Peter B, Längst Gernot

机构信息

Adolf-Butenandt-Institut, Molekularbiologie, Ludwig Maximilians Universität, 80336 Munich. German.

出版信息

Mol Cell Biol. 2004 Feb;24(4):1791-8. doi: 10.1128/MCB.24.4.1791-1798.2004.

DOI:10.1128/MCB.24.4.1791-1798.2004
PMID:14749393
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC344174/
Abstract

The rRNA gene cluster consists of multiple transcription units. Half of these are active, while the other half are transcriptionally inactive. Previously, in vivo studies have demonstrated that silencing of ribosomal DNA (rDNA) is mediated by the chromatin remodeling NoRC (nucleolar remodeling complex). To explore the mechanisms underlying NoRC-directed silencing of rDNA transcription, we investigated the effect of recombinant NoRC on RNA polymerase I transcription on reconstituted chromatin templates. We show that NoRC interacts with the transcription terminator factor (TTF-I), and this interaction is required both for the binding of TTF-I to its promoter-proximal target site and for the recruitment of NoRC to the promoter. After association with the rDNA promoter, NoRC alters the position of the promoter-bound nucleosome, thereby repressing RNA polymerase I transcription. This NoRC-directed rDNA repression requires the N terminus of histone H4. Repression is effective before preinitiation complex formation and as such is unable to exert an effect upon activated rDNA genes. Furthermore, the early steps of rDNA repression do not depend on DNA and histone modifications. These results reveal an important role for TTF-I in recruiting NoRC to rDNA and an active role for NoRC in the establishment of rDNA silencing.

摘要

核糖体RNA(rRNA)基因簇由多个转录单元组成。其中一半是活跃的,而另一半则是转录不活跃的。此前,体内研究表明,核糖体DNA(rDNA)的沉默是由染色质重塑复合物NoRC(核仁重塑复合物)介导的。为了探究NoRC介导的rDNA转录沉默的潜在机制,我们研究了重组NoRC对重组染色质模板上RNA聚合酶I转录的影响。我们发现NoRC与转录终止因子(TTF-I)相互作用,这种相互作用对于TTF-I与其启动子近端靶位点的结合以及NoRC募集到启动子上都是必需的。与rDNA启动子结合后,NoRC改变了与启动子结合的核小体的位置,从而抑制RNA聚合酶I转录。这种由NoRC介导的rDNA抑制需要组蛋白H4的N末端。抑制在起始前复合物形成之前就有效,因此对已激活的rDNA基因无法发挥作用。此外,rDNA抑制的早期步骤不依赖于DNA和组蛋白修饰。这些结果揭示了TTF-I在将NoRC募集到rDNA上的重要作用以及NoRC在建立rDNA沉默中的积极作用。