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A review of metabolic and enzymatic engineering strategies for designing and optimizing performance of microbial cell factories

机译:设计和优化微生物细胞工厂性能的代谢和酶促工程策略综述

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摘要

Microbial cell factories (MCFs) are of considerable interest to convert low value renewable substrates to biofuels and high value chemicals. This review highlights the progress of computational models for the rational design of an MCF to produce a target bio-commodity. In particular, the rational design of an MCF involves: (i) product selection, (ii) de novo biosynthetic pathway identification (i.e., rational, heterologous, or artificial), (iii) MCF chassis selection, (iv) enzyme engineering of promiscuity to enable the formation of new products, and (v) metabolic engineering to ensure optimal use of the pathway by the MCF host. Computational tools such as (i) de novo biosynthetic pathway builders, (ii) docking, (iii) molecular dynamics (MD) and steered MD (SMD), and (iv) genome-scale metabolic flux modeling all play critical roles in the rational design of an MCF. Genome-scale metabolic flux models are of considerable use to the design process since they can reveal metabolic capabilities of MCF hosts. These can be used for host selection as well as optimizing precursors and cofactors of artificial de novo biosynthetic pathways. In addition, recent advances in genome-scale modeling have enabled the derivation of metabolic engineering strategies, which can be implemented using the genomic tools reviewed here as well.
机译:微生物细胞工厂(MCF)对于将低价值的可再生底物转化为生物燃料和高价值的化学物质具有极大的兴趣。这篇评论重点介绍了用于合理设计MCF以生产目标生物商品的计算模型的进展。特别是,MCF的合理设计涉及:(i)产品选择,(ii)从头进行生物合成途径鉴定(即,合理,异源或人工),(iii)MCF底盘选择,(iv)滥交酶工程以形成新产品,以及(v)代谢工程以确保MCF宿主对途径的最佳利用。诸如(i)从头生物合成途径构建者,(ii)对接,(iii)分子动力学(MD)和操纵的MD(SMD)等计算工具,以及(iv)基因组规模的代谢通量建模均在理性中起关键作用MCF的设计。基因组规模的代谢通量模型可在设计过程中使用,因为它们可以揭示MCF宿主的代谢能力。这些可用于宿主选择以及优化人工从头生物合成途径的前体和辅因子。此外,基因组规模建模的最新进展使得能够推导代谢工程策略,也可以使用此处介绍的基因组工具来实施。

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