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NURD,一种兼具ATP依赖型染色质重塑和组蛋白去乙酰化酶活性的新型复合物。

NURD, a novel complex with both ATP-dependent chromatin-remodeling and histone deacetylase activities.

作者信息

Xue Y, Wong J, Moreno G T, Young M K, Côté J, Wang W

机构信息

Laboratory of Genetics, National Institute on Aging, National Institute of Health, Gerontology Research Center, Baltimore, Maryland 21224, USA.

出版信息

Mol Cell. 1998 Dec;2(6):851-61. doi: 10.1016/s1097-2765(00)80299-3.

Abstract

ATP-dependent chromatin-remodeling complexes are known to facilitate transcriptional activation by opening chromatin structures. We report a novel human complex, named NURD, which contains not only ATP-dependent nucleosome disruption activity, but also histone deacetylase activity, which usually associates with transcriptional repression. The deacetylation is stimulated by ATP on nucleosomal templates, suggesting that nucleosome disruption aids the deacetylase to access its substrates. One subunit of NURD was identified as MTA1, a metastasis-associated protein with a region similar to the nuclear receptor core-pressor, N-CoR; and antibodies against NURD partially relieve transcriptional repression by thyroid hormone receptor. These results suggest that ATP-dependent chromatin remodeling can participate in transcriptional repression by assisting repressors in gaining access to chromatin.

摘要

已知依赖ATP的染色质重塑复合物通过打开染色质结构促进转录激活。我们报道了一种新型人类复合物,命名为NURD,它不仅具有依赖ATP的核小体破坏活性,还具有通常与转录抑制相关的组蛋白脱乙酰酶活性。在核小体模板上,ATP可刺激去乙酰化作用,这表明核小体破坏有助于脱乙酰酶接近其底物。NURD的一个亚基被鉴定为MTA1,一种与转移相关的蛋白质,其一个区域类似于核受体共抑制因子N-CoR;针对NURD的抗体可部分缓解甲状腺激素受体的转录抑制作用。这些结果表明,依赖ATP的染色质重塑可通过协助抑制因子接近染色质来参与转录抑制。

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