首页> 外文期刊>Journal of biomolecular screening: The official journal of the Society for Biomolecular Screening >Fluorescence-Based Methods for Screening Writers and Readers of Histone Methyl Marks
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Fluorescence-Based Methods for Screening Writers and Readers of Histone Methyl Marks

机译:基于荧光的组蛋白甲基标记作者和读者筛选方法

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摘要

The histone methyltransferase (HMT) family of proteins consists of enzymes that methylate lysine or arginine residues on histone tails as well as other proteins. Such modifications affect chromatin structure and play a significant regulatory role in gene expression. Many HMTs have been implicated in tumorigenesis and progression of multiple malignancies and play essential roles in embryonic development and stem cell renewal. Overexpression of some HMTs has been observed and is correlated positively with various types of cancer. Here the authors report development of a continuous fluorescence-based methyltransferase assay in a 384-well format and its application in determining kinetic parameters for EHMT1, G9a, PRMT3, SETD7, and SUV39H2 as well as for screening against libraries of small molecules to identify enzyme inhibitors. They also report the development of a peptide displacement assay using fluorescence polarization in a 384-well format to assay and screen protein peptide interactions such as those of WDR5 and EED, components of MLL and EZH2 methyltransferase complexes. Using these high-throughput screening methods, the authors have identified potent inhibitors and ligands for some of these proteins.
机译:组蛋白甲基转移酶(HMT)家族的蛋白质由对组蛋白尾巴上的赖氨酸或精氨酸残基甲基化的酶以及其他蛋白质组成。这种修饰影响染色质结构,并在基因表达中起重要的调节作用。许多HMT已与多种恶性肿瘤的发生和发展有关,并在胚胎发育和干细胞更新中起着重要作用。已经观察到某些HMT的过度表达,并且与各种类型的癌症呈正相关。在这里,作者报告了一种基于384孔格式的基于连续荧光的甲基转移酶测定方法的开发,并将其应用于确定EHMT1,G9a,PRMT3,SETD7和SUV39H2的动力学参数,以及针对小分子文库进行筛选以鉴定酶抑制剂。他们还报告了使用384孔格式的荧光偏振进行肽置换分析的方法的开发,以分析和筛选蛋白质肽相互作用,例如WDR5和EED,MLL和EZH2甲基转移酶复合物的组分。使用这些高通量筛选方法,作者已经确定了其中某些蛋白质的有效抑制剂和配体。

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