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本文引用的文献

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Variations in several responses of HeLa cells to x-irradiation during the division cycle.在分裂周期中,海拉细胞对X射线照射的几种反应的变化。
Biophys J. 1963 Jan;3(1):11-33. doi: 10.1016/s0006-3495(63)86801-0.
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The Drosophila Polycomb group gene pleiohomeotic encodes a DNA binding protein with homology to the transcription factor YY1.果蝇的多梳基因pleiohomeotic编码一种与转录因子YY1具有同源性的DNA结合蛋白。
Mol Cell. 1998 Jun;1(7):1057-64. doi: 10.1016/s1097-2765(00)80106-9.
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Everything you have ever wanted to know about Yin Yang 1.....你一直想了解的关于阴阳1的一切……
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A conserved element in the protein-coding sequence is required for normal expression of replication-dependent histone genes in developing Xenopus embryos.在非洲爪蟾胚胎发育过程中,复制依赖性组蛋白基因的正常表达需要蛋白质编码序列中的一个保守元件。
Dev Biol. 1997 Feb 1;182(1):21-32. doi: 10.1006/dbio.1996.8459.
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Characterization of the transcriptional regulator YY1. The bipartite transactivation domain is independent of interaction with the TATA box-binding protein, transcription factor IIB, TAFII55, or cAMP-responsive element-binding protein (CPB)-binding protein.转录调节因子YY1的特性。双功能反式激活结构域与TATA盒结合蛋白、转录因子IIB、TAFII55或cAMP反应元件结合蛋白(CBP)-结合蛋白的相互作用无关。
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The protein that binds the 3' end of histone mRNA: a novel RNA-binding protein required for histone pre-mRNA processing.结合组蛋白mRNA 3'末端的蛋白质:一种组蛋白前体mRNA加工所需的新型RNA结合蛋白。
Genes Dev. 1996 Dec 1;10(23):3028-40. doi: 10.1101/gad.10.23.3028.
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An H3 coding region regulatory element is common to all four nucleosomal classes of mouse histone-encoding genes.
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Cell cycle-regulated binding of nuclear proteins to elements within a mouse H3.2 histone gene.细胞核蛋白与小鼠H3.2组蛋白基因内元件的细胞周期调控结合。
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Identification of a second conserved element within the coding sequence of a mouse H3 histone gene that interacts with nuclear factors and is necessary for normal expression.在小鼠H3组蛋白基因编码序列中鉴定出第二个保守元件,该元件与核因子相互作用,是正常表达所必需的。
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Induction of H3.3 replacement histone mRNAs during the precommitment period of murine erythroleukemia cell differentiation.在小鼠红白血病细胞分化的预决定期诱导H3.3替代组蛋白mRNA的产生。
Nucleic Acids Res. 1993 Jun 25;21(12):2873-9. doi: 10.1093/nar/21.12.2873.

YY1结合元件在依赖复制的小鼠组蛋白基因表达中的作用。

Role for a YY1-binding element in replication-dependent mouse histone gene expression.

作者信息

Eliassen K A, Baldwin A, Sikorski E M, Hurt M M

机构信息

Department of Biological Science, Florida State University, Tallahassee, Florida 32306-4370, USA.

出版信息

Mol Cell Biol. 1998 Dec;18(12):7106-18. doi: 10.1128/MCB.18.12.7106.

DOI:10.1128/MCB.18.12.7106
PMID:9819397
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC109292/
Abstract

Expression of the highly conserved replication-dependent histone gene family increases dramatically as a cell enters the S phase of the eukaryotic cell cycle. Requirements for normal histone gene expression in vivo include an element, designated alpha, located within the protein-encoding sequence of nucleosomal histone genes. Mutation of 5 of 7 nucleotides of the mouse H3.2 alpha element to yield the sequence found in an H3.3 replication-independent variant abolishes the DNA-protein interaction in vitro and reduces expression fourfold in vivo. A yeast one-hybrid screen of a HeLa cell cDNA library identified the protein responsible for recognition of the histone H3.2 alpha sequence as the transcription factor Yin Yang 1 (YY1). YY1 is a ubiquitous and highly conserved transcription factor reported to be involved in both activation and repression of gene expression. Here we report that the in vitro histone alpha DNA-protein interaction depends on YY1 and that mutation of the nucleotides required for the in vitro histone alpha DNA-YY1 interaction alters the cell cycle phase-specific up-regulation of the mouse H3.2 gene in vivo. Because all mutations or deletions of the histone alpha sequence both abolish interactions in vitro and cause an in vivo decrease in histone gene expression, the recognition of the histone alpha element by YY1 is implicated in the correct temporal regulation of replication-dependent histone gene expression in vivo.

摘要

高度保守的依赖复制的组蛋白基因家族的表达在细胞进入真核细胞周期的S期时会急剧增加。体内正常组蛋白基因表达的要求包括一个位于核小体组蛋白基因蛋白质编码序列内的元件,称为α元件。将小鼠H3.2α元件的7个核苷酸中的5个突变,以产生在H3.3非依赖复制变体中发现的序列,这在体外消除了DNA-蛋白质相互作用,并在体内使表达降低了四倍。对HeLa细胞cDNA文库进行酵母单杂交筛选,确定负责识别组蛋白H3.2α序列的蛋白质为转录因子阴阳1(YY1)。YY1是一种普遍存在且高度保守的转录因子,据报道它参与基因表达的激活和抑制。我们在此报告,体外组蛋白α DNA-蛋白质相互作用依赖于YY1,并且体外组蛋白α DNA-YY1相互作用所需核苷酸的突变会改变体内小鼠H3.2基因的细胞周期阶段特异性上调。由于组蛋白α序列的所有突变或缺失都会在体外消除相互作用,并导致体内组蛋白基因表达下降,因此YY1对组蛋白α元件的识别与体内依赖复制的组蛋白基因表达的正确时间调控有关。