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Design and engineering of artificial metalloproteins: from de novo metal coordination to catalysis

机译:人工金属蛋白的设计与工程:从De Novo金属协调到催化

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摘要

Metalloproteins are essential to sustain life. Natural evolution optimized them for intricate structural, regulatory and catalytic functions that cannot be fulfilled by either a protein or a metal ion alone. In order to understand this synergy and the complex design principles behind the natural systems, simpler mimics were engineered from the bottom up by installing de novo metal sites in either natural or fully designed, artificial protein scaffolds. This review focuses on key challenges associated with this approach. We discuss how proteins can be equipped with binding sites that provide an optimal coordination environment for a metal cofactor of choice, which can be a single metal ion or a complex multinuclear cluster. Furthermore, we highlight recent studies in which artificial metalloproteins were engineered towards newfunctions, including electron transfer and catalysis. In this context, the powerful combination of de novo protein design and directed evolution is emphasized for metalloenzyme development.
机译:金属蛋白是维持生命所必需的。自然进化优化了它们复杂的结构、调节和催化功能,而这些功能不是单靠蛋白质或金属离子就能实现的。为了理解这种协同作用以及自然系统背后的复杂设计原则,我们通过在自然或完全设计的人工蛋白质支架中安装从头开始的金属位点,从下到上设计了更简单的模拟物。本综述侧重于与此方法相关的关键挑战。我们讨论了蛋白质如何配备结合位点,为选择的金属辅因子(可以是单个金属离子或复杂的多核簇)提供最佳配位环境。此外,我们还重点介绍了最近的研究,其中人工金属蛋白被设计成新功能,包括电子转移和催化。在此背景下,金属酶的开发强调了从头蛋白质设计和定向进化的强大结合。

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