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首页> 外文期刊>Angewandte Chemie >Intracellular Reactions Promoted by Bis(histidine) Miniproteins Stapled Using Palladium(II) Complexes
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Intracellular Reactions Promoted by Bis(histidine) Miniproteins Stapled Using Palladium(II) Complexes

机译:通过双(组氨酸)促进的细胞内反应使用钯(II)复合物犯下的

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摘要

The generation of catalytically active metalloproteins inside living mammalian cells is a major research challenge at the interface between catalysis and cell biology. Herein we demonstrate that basic domains of bZIP transcription factors, mutated to include two histidine residues at i and i+4 positions, react with palladium(II) sources to generate catalytically active, stapled pallado-miniproteins. The resulting constrained peptides are efficiently internalized into living mammalian cells, where they perform palladium-promoted depropargylation reactions without cellular fixation. Control experiments confirm the requirement of the peptide scaffolding and the palladium staple for attaining the intracellular reactivity.
机译:生物哺乳动物细胞内催化活性金属蛋白的产生是催化和细胞生物学之间的界面处的主要研究挑战。 在此,我们证明BZIP转录因子的基本结构域突变为I和I + 4位的两个组氨酸残基,与钯(II)源反应,以产生催化活性的德斗普拉多微细胞蛋白。 所得约束的肽被有效地内化到活哺乳动物细胞中,在那里它们在没有细胞固定的情况下进行钯促进的面糊精反应。 对照实验证实了肽支架和钯钉以获得细胞内反应性的要求。

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