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人MLL5的PHD结构域的溶液核磁共振结构及组蛋白结合

Solution NMR structure and histone binding of the PHD domain of human MLL5.

作者信息

Lemak Alexander, Yee Adelinda, Wu Hong, Yap Damian, Zeng Hong, Dombrovski Ludmila, Houliston Scott, Aparicio Samuel, Arrowsmith Cheryl H

机构信息

Northeast Structural Genomics Consortium and Ontario Cancer Institute, University Health Network, Toronto, Ontario, Canada.

出版信息

PLoS One. 2013 Oct 9;8(10):e77020. doi: 10.1371/journal.pone.0077020. eCollection 2013.

Abstract

Mixed Lineage Leukemia 5 (MLL5) is a histone methyltransferase that plays a key role in hematopoiesis, spermatogenesis and cell cycle progression. In addition to its catalytic domain, MLL5 contains a PHD finger domain, a protein module that is often involved in binding to the N-terminus of histone H3. Here we report the NMR solution structure of the MLL5 PHD domain showing a variant of the canonical PHD fold that combines conserved H3 binding features from several classes of other PHD domains (including an aromatic cage) along with a novel C-terminal α-helix, not previously seen. We further demonstrate that the PHD domain binds with similar affinity to histone H3 tail peptides di- and tri-methylated at lysine 4 (H3K4me2 and H3K4me3), the former being the putative product of the MLL5 catalytic reaction. This work establishes the PHD domain of MLL5 as a bone fide 'reader' domain of H3K4 methyl marks suggesting that it may guide the spreading or further methylation of this site on chromatin.

摘要

混合谱系白血病5(MLL5)是一种组蛋白甲基转移酶,在造血、精子发生和细胞周期进程中发挥关键作用。除了其催化结构域外,MLL5还包含一个PHD指结构域,这是一种通常参与结合组蛋白H3 N端的蛋白质模块。在此,我们报道了MLL5 PHD结构域的核磁共振溶液结构,该结构显示了一种典型PHD折叠的变体,它结合了几类其他PHD结构域(包括一个芳香笼)的保守H3结合特征以及一个以前未见的新型C端α螺旋。我们进一步证明,PHD结构域与赖氨酸4二甲基化和三甲基化的组蛋白H3尾肽(H3K4me2和H3K4me3)具有相似的亲和力,前者是MLL5催化反应的假定产物。这项工作将MLL5的PHD结构域确立为H3K4甲基化标记的真正“读取”结构域,表明它可能指导该位点在染色质上的扩散或进一步甲基化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c6e5/3793974/89e285f3df22/pone.0077020.g001.jpg

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