甲基赖氨酸结合位点的成药性。

Druggability of methyl-lysine binding sites.

机构信息

Structural Genomics Consortium, University of Toronto, Toronto, ON, Canada.

出版信息

J Comput Aided Mol Des. 2011 Dec;25(12):1171-8. doi: 10.1007/s10822-011-9505-2. Epub 2011 Dec 7.

Abstract

Structural modules that specifically recognize--or read--methylated or acetylated lysine residues on histone peptides are important components of chromatin-mediated signaling and epigenetic regulation of gene expression. Deregulation of epigenetic mechanisms is associated with disease conditions, and antagonists of acetyl-lysine binding bromodomains are efficacious in animal models of cancer and inflammation, but little is known regarding the druggability of methyl-lysine binding modules. We conducted a systematic structural analysis of readers of methyl marks and derived a predictive druggability landscape of methyl-lysine binding modules. We show that these target classes are generally less druggable than bromodomains, but that some proteins stand as notable exceptions.

摘要

特异性识别组蛋白肽上甲基化或乙酰化赖氨酸残基的结构模块是染色质介导的信号转导和基因表达表观遗传调控的重要组成部分。表观遗传机制的失调与疾病状况有关，乙酰赖氨酸结合溴结构域的拮抗剂在癌症和炎症的动物模型中是有效的，但关于甲基赖氨酸结合模块的可药性知之甚少。我们对甲基标记的读取器进行了系统的结构分析，并得出了甲基赖氨酸结合模块的可预测性药物景观。我们表明，这些靶类通常比溴结构域的可药性差，但有些蛋白质则是显著的例外。

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甲基赖氨酸结合位点的成药性。

Druggability of methyl-lysine binding sites.

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