常染色质因子HULC和Set1C影响裂糖酵母异染色质组织和交配型转换。

IF 1 4区 生物学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY Genes & genetic systems Pub Date : 2022-10-18 DOI:10.1266/ggs.22-00012
Alfredo Esquivel-Chávez, Takahisa Maki, Hideo Tsubouchi, Testuya Handa, Hiroshi Kimura, James E Haber, Geneviève Thon, Hiroshi Iwasaki
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引用次数: 0

摘要

裂糖酵母(Schizosaccharomyces pombe)的交配型(P或M)由转录活性的mat1盒决定,并通过位于相邻异染色质区域的供体mat2或mat3的基因转换来切换(交配型切换;MTS)。在转换过程中,根据P或M细胞类型以及两种重组增强子(SRE2促进mat2-P的使用,SRE3促进mat3-M的使用)的作用选择遗传信息的异色供体,导致表达的mat1盒的内容被替换。最近,我们发现组蛋白H3K4甲基转移酶复合物Set1C参与供体选择,提出了一个以其在常染色质中的作用而闻名的复合物如何控制异染色质中的重组的问题。在这里,我们报道了组蛋白H2BK119泛素连接酶复合体HULC在MTS中与Set1C一起起作用,因为shf1、brl1、brl2和rad6基因的突变体表现出与Set1C突变体相似的缺陷,并且与set1Δ属于同一组。此外,利用H3K4R和H2BK119R组蛋白突变体以及Set1-Y897A催化突变体,我们发现在MTS中,HULC对组蛋白H2BK119的泛素化和Set1C对组蛋白H3K4的甲基化在功能上偶联,这些突变体在MTS中的细胞类型偏倚表明,HULC和Set1C抑制了M细胞中SRE3重组增强子的使用,从而有利于SRE2和mat2-P。与此一致,突变体中的不平衡开关可追溯到M细胞中方向性因子Swi6与重组增强子的关联受损。基于它们在其他染色体位置的已知作用,我们推测HULC和Set1C控制核小体的流动性和SRE元件附近的链入侵。此外,我们发现了HULC和Set1C对组蛋白H3K9甲基化和基因沉默的明显影响,这与异色结构域的其他功能一致。
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Euchromatin factors HULC and Set1C affect heterochromatin organization and mating-type switching in fission yeast Schizosaccharomyces pombe.

Mating-type (P or M) of fission yeast Schizosaccharomyces pombe is determined by the transcriptionally active mat1 cassette and is switched by gene conversion using a donor, either mat2 or mat3, located in an adjacent heterochromatin region (mating-type switching; MTS). In the switching process, heterochromatic donors of genetic information are selected based on the P or M cell type and on the action of two recombination enhancers, SRE2 promoting the use of mat2-P and SRE3 promoting the use of mat3-M, leading to replacement of the content of the expressed mat1 cassette. Recently, we found that the histone H3K4 methyltransferase complex Set1C participates in donor selection, raising the question of how a complex best known for its effects in euchromatin controls recombination in heterochromatin. Here, we report that the histone H2BK119 ubiquitin ligase complex HULC functions with Set1C in MTS, as mutants in the shf1, brl1, brl2 and rad6 genes showed defects similar to Set1C mutants and belonged to the same epistasis group as set1Δ. Moreover, using H3K4R and H2BK119R histone mutants and a Set1-Y897A catalytic mutant, we found that ubiquitylation of histone H2BK119 by HULC and methylation of histone H3K4 by Set1C are functionally coupled in MTS. Cell-type biases in MTS in these mutants suggested that HULC and Set1C inhibit the use of the SRE3 recombination enhancer in M cells, thus favoring SRE2 and mat2-P. Consistent with this, imbalanced switching in the mutants was traced to compromised association of the directionality factor Swi6 with the recombination enhancers in M cells. Based on their known effects at other chromosomal locations, we speculate that HULC and Set1C control nucleosome mobility and strand invasion near the SRE elements. In addition, we uncovered distinct effects of HULC and Set1C on histone H3K9 methylation and gene silencing, consistent with additional functions in the heterochromatic domain.

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来源期刊
Genes & genetic systems
Genes & genetic systems 生物-生化与分子生物学
CiteScore
1.50
自引率
0.00%
发文量
22
审稿时长
>12 weeks
期刊介绍: Genes & Genetic Systems , formerly the Japanese Journal of Genetics , is published bimonthly by the Genetics Society of Japan.
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