Cancer Research UK, London Research Institute, London, UK.
Nat Struct Mol Biol. 2010 Jul;17(7):862-8. doi: 10.1038/nsmb.1824. Epub 2010 Jun 13.
Several lines of evidence point to a role for noncoding RNA in transcriptional repression by Polycomb group (PcG) proteins, but the precise mechanism remains unclear. Here we show that human MOV10, a putative RNA helicase previously implicated in post-transcriptional gene silencing, co-purifies and interacts with components of Polycomb-repressive complex 1 (PRC1) from human cells. Endogenous human MOV10 is mostly nuclear, and a proportion associates with chromatin in an RNA-dependent manner. Small hairpin RNA (shRNA)-mediated knockdown of MOV10 in human fibroblasts leads to the upregulation of the INK4a tumor suppressor, a known target of PcG-mediated repression, accompanied by the dissociation of PRC1 proteins from the locus and a reduction in trimethylation of histone H3 on Lys27 (H3K27me3). As well as prompting reassessment of MOV10's role in other settings, our findings suggest that it is directly involved in transcriptional silencing by PcG complexes.
有几条证据表明非编码 RNA 在 Polycomb 组 (PcG) 蛋白的转录抑制中发挥作用,但确切的机制仍不清楚。在这里,我们表明人类 MOV10,一种先前被认为与转录后基因沉默有关的假定 RNA 解旋酶,与人细胞中的 Polycomb 抑制复合物 1 (PRC1) 的成分共纯化和相互作用。内源性人 MOV10 主要存在于核内,一部分以 RNA 依赖的方式与染色质结合。短发夹 RNA (shRNA)介导的人成纤维细胞中 MOV10 的敲低导致 INK4a 肿瘤抑制因子的上调,这是 PcG 介导的抑制的已知靶点,伴随着 PRC1 蛋白从基因座上解离以及组蛋白 H3 在赖氨酸 27 上的三甲基化 (H3K27me3) 减少。除了促使重新评估 MOV10 在其他环境中的作用外,我们的发现还表明它直接参与 PcG 复合物的转录沉默。
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