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泛特异性和部分选择性的多梳蛋白同源物的肽类抑制剂的染料标记物。

Pan-specific and partially selective dye-labeled peptidic inhibitors of the polycomb paralog proteins.

机构信息

Department of Chemistry, University of Victoria, Victoria, BC V8W 3V6, Canada.

BC Cancer - Trev and Joyce Deeley Research Centre, Victoria, BC V8R 6V5, Canada.

出版信息

Bioorg Med Chem. 2020 Jan 1;28(1):115176. doi: 10.1016/j.bmc.2019.115176. Epub 2019 Nov 9.

Abstract

Epigenetic regulation of gene expression is in part controlled by post-translational modifications on histone proteins. Histone methylation is a key epigenetic mark that controls gene transcription and repression. There are five human polycomb paralog proteins (Cbx2/4/6/7/8) that use their chromodomains to recognize trimethylated lysine 27 on histone 3 (H3K27me3). Recognition of the methyllysine side chain is achieved through multiple cation-pi interactions within an 'aromatic cage' motif. Despite high structural similarity within the chromodomains of this protein family, they each have unique functional roles and are linked to different cancers. Selective inhibition of different CBX proteins is desirable for both fundamental studies and potential therapeutic applications. We report here on a series of peptidic inhibitors that target certain polycomb paralogs. We have identified peptidic scaffolds with sub-micromolar potency, and will report examples that are pan-specific and that are partially selective for individual members within the family. These results highlight important structure-activity relationships that allow for differential binding to be achieved through interactions outside of the methyllysine-binding aromatic cage motif.

摘要

基因表达的表观遗传调控部分受组蛋白翻译后修饰控制。组蛋白甲基化是一种关键的表观遗传标记,可控制基因转录和抑制。有五个人类多梳蛋白同源物(Cbx2/4/6/7/8),它们利用其 chromodomains 识别组蛋白 3 上的三甲基赖氨酸 27(H3K27me3)。通过“芳香笼”基序内的多个阳离子-π相互作用实现对甲基赖氨酸侧链的识别。尽管该蛋白家族的 chromodomains 具有高度结构相似性,但它们各自具有独特的功能作用,并与不同的癌症相关。针对不同的 CBX 蛋白选择性抑制对于基础研究和潜在的治疗应用都是可取的。我们在这里报告了一系列针对某些多梳蛋白同源物的肽类抑制剂。我们已经确定了具有亚微摩尔效力的肽骨架,并将报告对泛特异性和对家族内个别成员具有部分选择性的例子。这些结果突出了重要的结构-活性关系,通过芳香笼基序之外的相互作用实现了差异结合。

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