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细菌微区室中的货物封装:方法与分析。

Cargo encapsulation in bacterial microcompartments: Methods and analysis.

作者信息

Nichols Taylor M, Kennedy Nolan W, Tullman-Ercek Danielle

机构信息

Department of Chemical and Biological Engineering, Northwestern University, Technological Institute, Evanston, IL, United States.

Interdisciplinary Biological Sciences Graduate Program, Northwestern University, Evanston, IL, United States.

出版信息

Methods Enzymol. 2019;617:155-186. doi: 10.1016/bs.mie.2018.12.009. Epub 2019 Feb 10.

Abstract

Metabolic engineers seek to produce high-value products from inexpensive starting materials in a sustainable and cost-effective manner by using microbes as cellular factories. However, pathway development and optimization can be arduous tasks, complicated by pathway bottlenecks and toxicity. Pathway organization has emerged as a potential solution to these issues, and the use of protein- or DNA-based scaffolds has successfully increased the production of several industrially relevant compounds. These efforts demonstrate the usefulness of pathway colocalization and spatial organization for metabolic engineering applications. In particular, scaffolding within an enclosed, subcellular compartment shows great promise for pathway optimization, offering benefits such as increased local enzyme and substrate concentrations, sequestration of toxic or volatile intermediates, and alleviation of cofactor and resource competition with the host. Here, we describe the 1,2-propanediol utilization (Pdu) bacterial microcompartment (MCP) as an enclosed scaffold for pathway sequestration and organization. We first describe methods for controlling Pdu MCP formation, expressing and encapsulating heterologous cargo, and tuning cargo loading levels. We further describe assays for analyzing Pdu MCPs and assessing encapsulation levels. These methods will enable the repurposing of MCPs as tunable nanobioreactors for heterologous pathway encapsulation.

摘要

代谢工程师试图以可持续且具有成本效益的方式,利用微生物作为细胞工厂,从廉价的起始原料生产高价值产品。然而,途径开发和优化可能是艰巨的任务,会受到途径瓶颈和毒性的困扰。途径组织已成为解决这些问题的潜在方法,基于蛋白质或DNA的支架的使用已成功提高了几种工业相关化合物的产量。这些努力证明了途径共定位和空间组织在代谢工程应用中的有用性。特别是,在封闭的亚细胞区室中进行支架构建对途径优化显示出巨大的潜力,具有提高局部酶和底物浓度、隔离有毒或挥发性中间体以及减轻与宿主的辅因子和资源竞争等优点。在此,我们描述了1,2-丙二醇利用(Pdu)细菌微区室(MCP)作为用于途径隔离和组织的封闭支架。我们首先描述控制Pdu MCP形成、表达和封装异源货物以及调节货物装载水平的方法。我们进一步描述用于分析Pdu MCPs和评估封装水平的测定方法。这些方法将使MCPs能够重新用作用于异源途径封装的可调谐纳米生物反应器。

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