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SET 结构域蛋白中的一个基序可结合单链核酸、转录 DNA 和超螺旋 DNA,并能干扰核小体的组装。

A motif within SET-domain proteins binds single-stranded nucleic acids and transcribed and supercoiled DNAs and can interfere with assembly of nucleosomes.

作者信息

Krajewski Wladyslaw A, Nakamura Tatsuya, Mazo Alexander, Canaani Eli

机构信息

Department of Biochemistry, Institute of Developmental Biology, Russian Academy of Sciences, Vavilova Str. 26, 117808 Moscow, Russia.

出版信息

Mol Cell Biol. 2005 Mar;25(5):1891-9. doi: 10.1128/MCB.25.5.1891-1899.2005.

Abstract

The evolutionary conserved SET domain is present in many eukaryotic chromatin-associated proteins, including some members of the trithorax (TrxG) group and the polycomb (PcG) group of epigenetic transcriptional regulators and modifiers of position effect variegation. All SET domains examined exhibited histone lysine methyltransferase activity, implicating these proteins in the generation of epigenetic marks. However, the mode of the initial recruitment of SET proteins to target genes and the way that their association with the genes is maintained after replication are not known. We found that SET-containing proteins of the SET1 and SET2 families contain motifs in the pre-SET region or at the pre-SET-SET and SET-post-SET boundaries which very tightly bind single-stranded DNA (ssDNA) and RNA. These motifs also bind stretches of ssDNA generated by superhelical tension or during the in vitro transcription of duplex DNA. Importantly, such binding withstands nucleosome assembly, interfering with the formation of regular nucleosomal arrays. Two representatives of the SUV39 SET family, SU(VAR)3-9 and G9a, did not bind ssDNA. The trxZ11 homeotic point mutation, which is located within TRX SET and disrupts embryonic development, impairs the ssDNA binding capacity of the protein. We suggest that the motifs described here may be directly involved in the biological function(s) of SET-containing proteins. The binding of single-stranded nucleic acids might play a role in the initial recruitment of the proteins to target genes, in the maintenance of their association after DNA replication, or in sustaining DNA stretches in a single-stranded configuration to allow for continuous transcription.

摘要

进化保守的SET结构域存在于许多真核生物染色质相关蛋白中,包括三胸节(TrxG)组和多梳(PcG)组的一些成员,这些都是表观遗传转录调节因子和位置效应斑驳修饰因子。所有检测的SET结构域都表现出组蛋白赖氨酸甲基转移酶活性,这表明这些蛋白参与了表观遗传标记的产生。然而,SET蛋白最初募集到靶基因的方式以及复制后它们与基因的结合维持方式尚不清楚。我们发现,SET1和SET2家族中含SET的蛋白在SET前区域或SET前-SET和SET后-SET边界处含有基序,这些基序能非常紧密地结合单链DNA(ssDNA)和RNA。这些基序也能结合由超螺旋张力产生的或双链DNA体外转录过程中产生的ssDNA片段。重要的是,这种结合能抵抗核小体组装,干扰规则核小体阵列的形成。SUV39 SET家族的两个代表,SU(VAR)3-9和G9a,不结合ssDNA。位于TRX SET内并破坏胚胎发育的trxZ11同源异型点突变会损害该蛋白的ssDNA结合能力。我们认为这里描述的基序可能直接参与含SET蛋白的生物学功能。单链核酸的结合可能在蛋白质最初募集到靶基因、DNA复制后维持它们的结合或维持DNA片段处于单链构象以允许连续转录中发挥作用。

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