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首页> 外文期刊>Angewandte Chemie >Tailoring Chimeric Ligands for Studying and Biasing ErbB Receptor Family Interactions
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Tailoring Chimeric Ligands for Studying and Biasing ErbB Receptor Family Interactions

机译:量身定制嵌合配体,以研究和减轻ErbB受体家族的相互作用。

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Described is the development and application of a versatile semisynthetic strategy, based on a combination of sortase-mediated coupling and tetrazine ligation chemistry, which can be exploited for the efficient incorporation of tunable functionality into chimeric recombinant proteins. To demonstrate the scope of the method, the assembly of a set of bivalent ligands, which integrate members of the epidermal growth factor (EGF) ligand family, is described. By using a series of bivalent EGFs with variable intraligand spacing, the differences in structure were correlated with the ability to bias signaling in the ErbB receptor family in a cell motility assay. Biasing away from EGFR-HER2 dimerization with a bivalent EGF was observed to reduce cell motility in an intraligand distance-dependent fashion, thus demonstrating the utility of the approach for acutely perturbing receptor-mediated cell signaling pathways.
机译:描述了基于分选酶介导的偶联和四嗪连接化学的组合的多功能半合成策略的开发和应用,可以将其用于将可调功能性有效地掺入嵌合重组蛋白中。为了证明该方法的范围,描述了整合表皮生长因子(EGF)配体家族成员的一组二价配体的组装。通过使用一系列具有可变配体内间隔的二价EGF,在细胞运动性测定中,结构差异与ErbB受体家族中偏向信号传导的能力相关。观察到用二价EGF消除EGFR-HER2二聚化的倾向以配体内距离依赖性方式降低细胞运动性,从而证明了该方法可用于急性扰动受体介导的细胞信号通路。

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