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本文引用的文献

1
The iab-7 polycomb response element maps to a nucleosome-free region of chromatin and requires both GAGA and pleiohomeotic for silencing activity.iab-7 多梳反应元件定位于染色质的无核小体区域,并且沉默活性需要 GAGA 和多效同源蛋白两者。
Mol Cell Biol. 2001 Feb;21(4):1311-8. doi: 10.1128/MCB.21.4.1311-1318.2001.
2
Sex determination in the Drosophila germline is dictated by the sexual identity of the surrounding soma.果蝇生殖系中的性别决定由周围体细胞的性别特征决定。
Genetics. 2000 Aug;155(4):1741-56. doi: 10.1093/genetics/155.4.1741.
3
Functional mapping of the GAGA factor assigns its transcriptional activity to the C-terminal glutamine-rich domain.GAGA因子的功能图谱将其转录活性定位到富含谷氨酰胺的C末端结构域。
J Biol Chem. 2000 Jun 30;275(26):19461-8. doi: 10.1074/jbc.M000967200.
4
Structure of a polycomb response element and in vitro binding of polycomb group complexes containing GAGA factor.多梳反应元件的结构以及包含GAGA因子的多梳蛋白复合体的体外结合
Mol Cell Biol. 2000 May;20(9):3187-97. doi: 10.1128/MCB.20.9.3187-3197.2000.
5
The Zw5 protein, a component of the scs chromatin domain boundary, is able to block enhancer-promoter interaction.Zw5蛋白是scs染色质结构域边界的一个组成部分,能够阻断增强子与启动子的相互作用。
Genes Dev. 1999 Aug 15;13(16):2098-107. doi: 10.1101/gad.13.16.2098.
6
Analysis of the doublesex female protein in Drosophila melanogaster: role on sexual differentiation and behavior and dependence on intersex.黑腹果蝇中双性雌性蛋白的分析:对性别分化和行为的作用以及对雌雄间性的依赖性
Genetics. 1999 Aug;152(4):1653-67. doi: 10.1093/genetics/152.4.1653.
7
The glutamine-rich domain of the Drosophila GAGA factor is necessary for amyloid fibre formation in vitro, but not for chromatin remodelling.
J Mol Biol. 1999 Jan 15;285(2):527-44. doi: 10.1006/jmbi.1998.2355.
8
DNA distortion and multimerization: novel functions of the glutamine-rich domain of GAGA factor.DNA扭曲与多聚化:GAGA因子富含谷氨酰胺结构域的新功能。
J Mol Biol. 1999 Jan 15;285(2):515-25. doi: 10.1006/jmbi.1998.2356.
9
GAGA mediates the enhancer blocking activity of the eve promoter in the Drosophila embryo.GAGA介导了果蝇胚胎中eve启动子的增强子阻断活性。
Genes Dev. 1998 Nov 1;12(21):3325-30. doi: 10.1101/gad.12.21.3325.
10
Comparison of the GAGA factor genes of Drosophila melanogaster and Drosophila virilis reveals high conservation of GAGA factor structure beyond the BTB/POZ and DNA-binding domains.黑腹果蝇和粗壮果蝇GAGA因子基因的比较揭示了GAGA因子结构在BTB/POZ和DNA结合结构域之外具有高度保守性。
Dev Genes Evol. 1998 Oct;208(8):447-56. doi: 10.1007/s004270050202.

GAGA因子亚型在体内具有不同但重叠的功能。

GAGA factor isoforms have distinct but overlapping functions in vivo.

作者信息

Greenberg A J, Schedl P

机构信息

Dept. of Molecular Biology, Princeton University, Princeton, NJ 08544, USA.

出版信息

Mol Cell Biol. 2001 Dec;21(24):8565-74. doi: 10.1128/MCB.21.24.8565-8574.2001.

DOI:10.1128/MCB.21.24.8565-8574.2001
PMID:11713290
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC100018/
Abstract

The Drosophila melanogaster GAGA factor (encoded by the Trithorax-like [Trl] gene) is required for correct chromatin architecture at diverse chromosomal sites. The Trl gene encodes two alternatively spliced isoforms of the GAGA factor (GAGA-519 and GAGA-581) that are identical except for the length and sequence of the C-terminal glutamine-rich (Q) domain. In vitro and tissue culture experiments failed to find any functional difference between the two isoforms. We made a set of transgenes that constitutively express cDNAs coding for either of the isoforms with the goal of elucidating their roles in vivo. Phenotypic analysis of the transgenes in Trl mutant background led us to the conclusion that GAGA-519 and GAGA-581 perform different, albeit largely overlapping, functions. We also expressed a fusion protein with LacZ disrupting the Q domain of GAGA-519. This LacZ fusion protein compensated for the loss of wild-type GAGA factor to a surprisingly large extent. This suggests that the Q domain either is not required for the essential functions performed by the GAGA protein or is exclusively used for tetramer formation. These results are inconsistent with a major role of the Q domain in chromatin remodeling or transcriptional activation. We also found that GAGA-LacZ was able to associate with sites not normally occupied by the GAGA factor, pointing to a role of the Q domain in binding site choice in vivo.

摘要

果蝇的GAGA因子(由类三胸蛋白基因[Trl]编码)对于不同染色体位点的正确染色质结构是必需的。Trl基因编码GAGA因子的两种选择性剪接异构体(GAGA-519和GAGA-581),除了C末端富含谷氨酰胺(Q)结构域的长度和序列外,它们是相同的。体外和组织培养实验未能发现这两种异构体之间有任何功能差异。我们构建了一组转基因,它们组成性地表达编码这两种异构体之一的cDNA,目的是阐明它们在体内的作用。对Trl突变背景下转基因的表型分析使我们得出结论,GAGA-519和GAGA-581执行不同的功能,尽管在很大程度上有重叠。我们还表达了一种与LacZ融合的蛋白,该蛋白破坏了GAGA-519的Q结构域。这种LacZ融合蛋白在很大程度上补偿了野生型GAGA因子的缺失。这表明Q结构域对于GAGA蛋白执行的基本功能不是必需的,或者专门用于四聚体形成。这些结果与Q结构域在染色质重塑或转录激活中的主要作用不一致。我们还发现GAGA-LacZ能够与GAGA因子通常不占据的位点结合,这表明Q结构域在体内结合位点选择中起作用。