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A Scalable Platform for Producing Recombinant Nucleosomes with Codified Histone Methyltransferase Substrate Preferences

机译:一种可伸缩平台,用于生产具有编纂组甲基转移酶基质偏好的重组核体

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摘要

Wolf-Hirschhorn Syndrome Candidate 1 (WHSC1; also known as NSD2) is a SET domain-containing histone lysine methyltransferase. A chromosomal translocation occurs in 15-20% of multiple myeloma patients and is associated with increased production of WHSC1 and poor clinical prognosis. To define the substrate requirements of NSD2, we established a platform for the large-scale production of recombinant polynucleosomes, based on authentic human histone proteins, expressed in E. coli, and complexed with linearized DNA. A brief survey of methyltransferases whose substrate requirements are recorded in the literature yielded expected results, lending credence to the fitness of our approach. This platform was readily 'codified' with respect to both position and extent of methylation at histone 3 lysines 18 and 36 and led to the conclusion that the most readily discernible activity of NSD2 in contact with a nucleosome substrate is dimethylation of histone 3 lysine 36. We further explored reaction mechanism, and conclude a processive, rather than distributive mechanism best describes the interaction of NSD2 with intact nucleosome substrates. The methods developed feature scale and flexibility and are suited to thorough pharmaceutical-scale drug discovery campaigns.
机译:Wolf-Hirschhorn综合征候选1(WHSC1;也称为NSD2)是含有结构域的组氨酸赖氨酸甲基转移酶。染色体易位发生在15-20%的多发性骨髓瘤患者中,并且与WHSC1的产量增加以及临床预后不良相关。为了定义NSD2的基材要求,我们建立了基于正宗人类组蛋白的重组多核体的大规模产生的平台,在大肠杆菌中表达,并用线性化DNA络合。简要调查甲基转移酶的基材要求在文献中记录的结果产生了预期的结果,贷款对我们方法的适应性。该平台在组蛋白3赖氨酸18和36处的甲基化的位置和程度易于“编纂”,并导致结论,NSD2与核体基质接触的最容易可辨别的活性是组蛋白3赖氨酸36的二甲基化。我们进一步探索了反应机制,并得出了分配机制,而不是分配机制最能描述NSD2与完整的核心基质的相互作用。该方法开发了特征规模和灵活性,适用于彻底的药学规模药物发现活动。

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