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Rtt106p is a histone chaperone involved in heterochromatin-mediated silencing

机译:Rtt106p是一种组蛋白伴侣,参与异染色质介导的沉默

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Epigenetic inheritance of heterochromatin structure is an important cellular process whose mechanism remains elusive. In this article, we describe the identification of nine enhancers of the silencing defect of a Saccharomyces cerevisiae-PCNA mutant by screening a library of approximate to 4,700 viable yeast deletion mutants. Of the nine mutants identified, six (hir1, hir3, sas2, sas4, sas5, and sir1) were previously known to reduce silencing synergistically with a mutation in Cac1p, the large subunit of chromatin assembly factor 1 (CAF-1). The predicted gene products that are affected in three other mutants (nam7, msh2, and rtt106) have not been implicated previously in silencing. Characterization of the rtt106 Delta allele revealed that it synergistically reduced heterochromatin silencing when combined with a mutation in Cac1p but not with a mutation in Asf1p (a histone H3 and H4 chaperone). Moreover, Rtt106p interacted with histories H3 and H4 both in vitro and in vivo, and it displayed a nucleosome assembly activity in vitro. Furthermore, Rtt106p interacts with CAF-1 physically through Cac1p. These biochemical and genetic data indicate that Rtt106p is a previously uncharacterized histone chaperone connecting S phase to epigenetic inheritance.
机译:异染色质结构的表观遗传是一个重要的细胞过程,其机制尚不清楚。在本文中,我们通过筛选大约4700个有生命的酵母缺失突变体的文库,描述了酿酒酵母-PCNA突变体沉默缺陷的九种增强子的鉴定。在确定的九种突变体中,先前已知六种(hir1,hir3,sas2,sas4,sas5和sir1)可与染色质装配因子1(CAF-1)的大亚基Cac1p突变协同降低沉默。先前尚未涉及沉默的其他三个突变体(nam7,msh2和rtt106)中受影响的预测基因产物。 rtt106 Delta等位基因的表征显示,与Cac1p中的突变结合但与Asf1p中的突变(组蛋白H3和H4分子伴侣)结合时,它协同降低异染色质沉默。此外,Rtt106p在体外和体内均与历史H3和H4相互作用,并且在体外显示出核小体装配活性。此外,Rtt106p通过Cac1p与CAF-1进行物理交互。这些生化和遗传数据表明,Rtt106p是先前未表征的组蛋白伴侣,将S期连接至表观遗传。

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