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General Chemoselective and Redox-Responsive Ligationand Release Strategy

机译:一般的化学选择性和氧化还原反应结扎和发布策略

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摘要

We report a switchable redox click and cleave reaction strategy for conjugating and releasing a range of molecules on demand. This chemoselective redox-responsive ligation (CRRL) and release strategy is based on a redox switchable oxime linkage that is controlled by mild chemical or electrochemical redox signals and can be performed at physiological conditions without the use of a catalyst. Both conjugation and release reactions are kinetically well behaved and quantitative. The CRRL strategy is synthetically modular and easily monitored and characterized by routine analytical techniques. We demonstrate how the CRRL strategy can be used for the dynamic generation of cyclic peptides and the ligation of two different peptides that are stable but can be selectively cleaved upon changes in the redox environment. We also demonstrate a new redox based delivery of cargoes to live cells strategy via the CRRL methodology by synthesizing a FRET redox-responsive probe that is selectively activated within a cellular environment. We believe the ease of the CRRL strategy should find wide use in a range of applicationsin biology, tissue engineering, nanoscience, synthetic chemistry,and material science and will expand the suite of current conjugationand release strategies.
机译:我们报告了一种可切换的氧化还原点击和裂解反应策略,用于根据需要缀合和释放一系列分子。这种化学选择性氧化还原响应性连接(CRRL)和释放策略基于氧化还原可转换肟键,该键由温和的化学或电化学氧化还原信号控制,可以在生理条件下进行而无需使用催化剂。缀合和释放反应均在动力学上表现良好且定量。 CRRL策略是综合模块化的,可以通过常规分析技术轻松监控和表征。我们演示了如何将CRRL策略用于动态生成环肽以及连接两个稳定但可以在氧化还原环境变化时选择性裂解的不同肽。我们还演示了通过合成通过在细胞环境中选择性激活的FRET氧化还原响应探针,通过CRRL方法​​论向载货细胞转移到活细胞策略的基于氧化还原的新方法。我们相信CRRL策略的简便性应在各种应用中得到广泛应用在生物学,组织工程,纳米科学,合成化学,和材料科学,并将扩展当前的结合套件和发布策略。

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