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Regulation of Acetylation at the Major Histocompatibility Complex Class II Proximal Promoter by the 19S Proteasomal ATPase Sug1

机译:19S蛋白酶体ATPase Sug1在主要组织相容性复合体II类近端启动子上乙酰化的调节。

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Recent studies have made evident the fact that the 19S regulatory component of the proteasome has functions that extend beyond degradation, particularly in the regulation of transcription. Although 19S ATPases facilitate chromatin remodeling and acetylation events in yeast (Saccharomyces cerevisiae), it is unclear if they play similar roles in mammalian cells. We have recently shown that the 19S ATPase Sug1 positively regulates the transcription of the critical inflammatory gene for major histocompatibility complex class II (MHC-II) by stabilizing enhanceosome assembly at the proximal promoter. We now show that Sug1 is crucial for regulating histone H3 acetylation at the MHC-II proximal promoter. Sug1 binds to acetylated histone H3 and, in the absence of Sug1, histone H3 acetylation is dramatically decreased at the proximal promoter, with a preferential loss of acetylation at H3 lysine 18. Sug1 also binds to the MHC-II histone acetyltransferase CREB-binding protein (CBP) and is critical for the recruitment of CBP to the MHC-II proximal promoter. Our current study strongly implicates the 19S ATPase Sug1 in modifying histones to initiate MHC-II transcription and provides novel insights into the role of the proteasome in the regulation of mammalian transcription.
机译:最近的研究表明,蛋白酶体的19S调控成分具有的功能不仅限于降解,还包括转录调控。尽管19S ATPases促进了酵母()中的染色质重塑和乙酰化事件,但尚不清楚它们是否在哺乳动物细胞中发挥相似的作用。我们最近显示19S ATPase Sug1通过稳定近端启动子的增强体组装,积极调节主要组织相容性复合物II类(MHC-II)的关键炎症基因的转录。现在,我们显示Sug1对于调节MHC-II近端启动子处的组蛋白H3乙酰化至关重要。 Sug1与乙酰化的组蛋白H3结合,并且在不存在Sug1的情况下,在近端启动子处组蛋白H3的乙酰化作用显着降低,在H3赖氨酸18处优先失去乙酰化。Sug1也与MHC-II组蛋白乙酰化转移酶CREB结合蛋白结合。 (CBP),对于将CBP募集到MHC-II近端启动子至关重要。我们当前的研究强烈暗示19S ATPase Sug1修饰组蛋白以启动MHC-II转录,并提供蛋白酶体在调节哺乳动物转录中的作用的新见解。

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