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在Zeste蛋白中存在一个富含脯氨酸的区域,该区域对于Zeste介导的转座作用和白色抑制至关重要。

A proline-rich region in the Zeste protein essential for transvection and white repression by Zeste.

作者信息

Rosen C, Dorsett D, Jack J

机构信息

Program in Molecular Biology, Sloan-Kettering Institute for Cancer Research, Memorial Sloan-Kettering Cancer Center, New York, New York 10021, USA.

出版信息

Genetics. 1998 Apr;148(4):1865-74. doi: 10.1093/genetics/148.4.1865.

Abstract

The DNA-binding protein encoded by the zeste gene of Drosophila activates transcription and mediates interchromosomal interactions such as transvection. The mutant protein encoded by the zeste1 (z1) allele retains the ability to support transvection, but represses white. Similar to transvection, repression requires Zeste-Zeste protein interactions and a second copy of white, either on the homologous chromosome or adjacent on the same chromosome. We characterized two pseudorevertants of z1 (z1-35 and z1-42) and another zeste mutation (z78c) that represses white. The z1 lesion alters a lysine residue located between the N-terminal DNA-binding domain and the C-terminal hydrophobic repeats involved in Zeste self-interactions. The z78c mutation alters a histidine near the site of the z1 lesion. Both z1 pseudorevertants retain the z1 lesion and alter different prolines in a proline-rich region located between the z1 lesion and the self-interaction domain. The pseudorevertants retain the ability to self-interact, but fail to repress white or support transvection at Ultrabithorax. To account for these observations and evidence indicating that Zeste affects gene expression through Polycomb group (Pc-G) protein complexes that epigenetically maintain chromatin states, we suggest that the regions affected by the z1, z78c, and pseudorevertant lesions mediate interactions between Zeste and the maintenance complexes.

摘要

果蝇zeste基因编码的DNA结合蛋白可激活转录并介导染色体间相互作用,如顺式效应。zeste1(z1)等位基因编码的突变蛋白保留了支持顺式效应的能力,但会抑制白色基因的表达。与顺式效应类似,抑制作用需要Zeste-Zeste蛋白相互作用以及白色基因的第二个拷贝,该拷贝位于同源染色体上或同一染色体上相邻位置。我们对z1的两个假回复突变体(z1-35和z1-42)以及另一个抑制白色基因表达的zeste突变(z78c)进行了表征。z1损伤改变了一个赖氨酸残基,该残基位于N端DNA结合结构域和参与Zeste自身相互作用的C端疏水重复序列之间。z78c突变改变了z1损伤位点附近的一个组氨酸。两个z1假回复突变体都保留了z1损伤,并改变了位于z1损伤和自身相互作用结构域之间富含脯氨酸区域的不同脯氨酸。这些假回复突变体保留了自我相互作用的能力,但无法抑制白色基因的表达或在超双胸基因处支持顺式效应。为了解释这些观察结果以及表明Zeste通过表观遗传维持染色质状态的多梳蛋白组(Pc-G)蛋白复合物影响基因表达的证据,我们认为受z1、z78c和假回复突变损伤影响的区域介导了Zeste与维持复合物之间的相互作用。

相似文献

10
The Drosophila zeste gene and transvection.果蝇小体基因与异位效应。
Trends Genet. 1989 Jun;5(6):189-94. doi: 10.1016/0168-9525(89)90074-7.

本文引用的文献

1
PcG complexes and chromatin silencing.多梳蛋白复合体与染色质沉默
Curr Opin Genet Dev. 1997 Apr;7(2):249-58. doi: 10.1016/s0959-437x(97)80135-9.
5
Propagating memory of transcriptional states.转录状态的记忆传递。
Trends Genet. 1995 Aug;11(8):295-7. doi: 10.1016/s0168-9525(00)89081-2.

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