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Directed evolution of biosynthetic pathways to carotenoids with unnatural carbon backbones.

机译:指导生物合成途径进化为具有非天然碳骨架的类胡萝卜素。

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Over the course of evolution, nature continually discovers new small molecules through the alteration of biosynthetic enzymes and pathways by mutation and gene transfer. Hundreds of these natural products have proven indispensable to medicine, culture, and technology, greatly contributing to increases in the length and quality of human lives. Chemists have found that the "chemical space" surrounding natural products is especially rich in functional molecules, and synthesis of natural product analogs has uncovered many with new or improved properties.; Inspired by nature's search algorithm, we and others have conducted our own evolution of carotenoid biosynthetic pathways in the laboratory. Chapter 1 comprehensively reviews the motivations, accomplishments, and challenges of this research area as of early 2005, and describes in detail how biosynthetic routes to dozens of new carotenoids have been established.; To expand the number of carotenoid backbones beyond the C30 and C40 carbon scaffolds that give rise to the ∼700 known natural carotenoids, we subjected a carotenoid synthase, the enzyme responsible for carotenoid backbone synthesis, to directed evolution. Chapter 2 describes the evolution of the C30 carotenoid synthase CrtM from Staphylococcus aureus for the ability to synthesize C40 carotenoids. This work also resulted in novel carotenoids with C35 backbones. We later found that some of the CrtM mutants generated in this laboratory evolution experiment, as well as several second-generation variants, are also capable of synthesizing unnatural C45 and C50 carotenoid backbones when supplied with appropriate prenyl diphosphate precursors.; Chapter 3 describes the creation of full-fledged pathways to carotenoid pigments based on the C45 and C50 scaffolds. Coexpression of the carotenoid desaturase CrtI from Erwinia uredovora resulted in the biosynthesis of at least 10 new C45 and C 50 carotenoids with different systems of conjugated double bonds. We also present evidence of an unnatural asymmetric C40 carotenoid pathway beginning with the condensation of farnesyl diphosphate (FPP, C15PP) and farnesylgeranyl diphosphate (FGPP, C25PP). In addition to clarifying how CrtM and CrtI achieve their product specificities, this work also sheds light on the molecular mechanisms used by evolution to access new chemical diversity and the selective pressures that have shaped natural product biosynthesis.
机译:在进化过程中,自然界不断通过突变和基因转移改变生物合成酶和途径,不断发现新的小分子。数以百计的这些天然产物已被证明对医学,文化和技术必不可少,极大地促进了人类寿命的延长和质量的提高。化学家发现,围绕天然产物的“化学空间”尤其富含功能分子,天然产物类似物的合成已发现许多具有新特性或改进特性的物质。受大自然搜索算法的启发,我们和其他人在实验室中进行了类胡萝卜素生物合成途径的进化。第1章从2005年初开始全面回顾了该研究领域的动机,成就和挑战,并详细介绍了如何建立通往数十种新类胡萝卜素的生物合成途径。为了将类胡萝卜素骨架的数量扩展到C30和C40碳支架之外,从而产生约700种已知的天然类胡萝卜素,我们对类胡萝卜素合酶(负责类胡萝卜素骨架合成的酶)进行了定向进化。第2章介绍了金黄色葡萄球菌C30类胡萝卜素合酶CrtM的进化,具有合成C40类胡萝卜素的能力。这项工作还产生了具有C35主链的新型类胡萝卜素。我们后来发现,在该实验室进化实验中产生的一些CrtM突变体,以及一些第二代变异体,在提供适当的异戊二烯基二磷酸前体时,也能够合成非天然的C45和C50类胡萝卜素骨架。第3章介绍了基于C45和C50支架建立类胡萝卜素色素的完整途径。来自美化欧文氏菌的类胡萝卜素去饱和酶CrtI的共表达导致至少10种具有不同共轭双键系统的新C45和C 50类胡萝卜素的生物合成。我们还提供了一个不自然的不对称C40类胡萝卜素途径的证据,该途径始于法呢基二磷酸(FPP,C15PP)和法呢基香叶基二磷酸(FGPP,C25PP)的缩合。除了阐明CrtM和CrtI如何实现其产品特异性外,这项工作还阐明了进化过程中使用的分子机制以获取新的化学多样性以及决定了天然产物生物合成的选择性压力。

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