首页> 外文期刊>Molecular cell >Histone chaperones ASF1 and NAP1 differentially modulate removal of active histone marks by LID-RPD3 complexes during NOTCH silencing.
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Histone chaperones ASF1 and NAP1 differentially modulate removal of active histone marks by LID-RPD3 complexes during NOTCH silencing.

机译:组蛋白伴侣ASF1和NAP1在NOTCH沉默过程中差异调节LID-RPD3复合物清除活性组蛋白标记的过程。

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摘要

Histone chaperones are involved in a variety of chromatin transactions. By a proteomics survey, we identified the interaction networks of histone chaperones ASF1, CAF1, HIRA, and NAP1. Here, we analyzed the cooperation of H3/H4 chaperone ASF1 and H2A/H2B chaperone NAP1 with two closely related silencing complexes: LAF and RLAF. NAP1 binds RPD3 and LID-associated factors (RLAF) comprising histone deacetylase RPD3, histone H3K4 demethylase LID/KDM5, SIN3A, PF1, EMSY, and MRG15. ASF1 binds LAF, a similar complex lacking RPD3. ASF1 and NAP1 link, respectively, LAF and RLAF to the DNA-binding Su(H)/Hairless complex, which targets the E(spl) NOTCH-regulated genes. ASF1 facilitates gene-selective removal of the H3K4me3 mark by LAF but has no effect on H3 deacetylation. NAP1 directs high nucleosome density near E(spl) control elements and mediates both H3 deacetylation and H3K4me3 demethylation by RLAF. We conclude that histone chaperones ASF1 and NAP1 differentially modulate local chromatin structure during gene-selective silencing.
机译:组蛋白伴侣参与各种染色质交易。通过蛋白质组学调查,我们确定了组蛋白伴侣ASF1,CAF1,HIRA和NAP1的相互作用网络。在这里,我们分析了H3 / H4分子伴侣ASF1和H2A / H2B分子伴侣NAP1与两个密切相关的沉默复合体:LAF和RLAF的协同作用。 NAP1结合包含组蛋白脱乙酰基酶RPD3,组蛋白H3K4脱甲基酶LID / KDM5,SIN3A,PF1,EMSY和MRG15的RPD3和LID相关因子(RLAF)。 ASF1结合LAF,这是缺少RPD3的类似复合物。 ASF1和NAP1分别将LAF和RLAF连接到DNA结合的Su(H)/无毛复合物,该复合物靶向E(spl)NOTCH调控的基因。 ASF1有助于通过LAF选择性去除H3K4me3标记,但对H3脱乙酰作用不起作用。 NAP1指导E(spl)控制元件附近的高核小体密度,并通过RLAF介导H3脱乙酰化和H3K4me3脱甲基。我们得出结论,在基因选择性沉默期间,组蛋白分子伴侣ASF1和NAP1差异性调节局部染色质结构。

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