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通过体外和体内代谢工程策略的偶联,人为设计将淀粉转化为增值甘露糖基化合物的途径。

Artificially designed routes for the conversion of starch to value-added mannosyl compounds through coupling in vitro and in vivo metabolic engineering strategies.

机构信息

University of Chinese Academy of Sciences, Beijing, 100049, China; National Engineering Laboratory for Industrial Enzymes, Tianjin Institute of Industrial Biotechnology, Chinese Academy of Sciences, Tianjin, 300308, China.

National Engineering Laboratory for Industrial Enzymes, Tianjin Institute of Industrial Biotechnology, Chinese Academy of Sciences, Tianjin, 300308, China.

出版信息

Metab Eng. 2020 Sep;61:215-224. doi: 10.1016/j.ymben.2020.06.008. Epub 2020 Jul 3.

Abstract

Starch/cellulose has become the major feedstock for manufacturing biofuels and biochemicals because of their abundance and sustainability. In this study, we presented an artificially designed "starch-mannose-fermentation" biotransformation process through coupling the advantages of in vivo and in vitro metabolic engineering strategies together. Starch was initially converted into mannose via an in vitro metabolic engineering biosystem, and then mannose was fermented by engineered microorganisms for biomanufacturing valuable mannosyl compounds. The in vitro metabolic engineering biosystem based on phosphorylation/dephosphorylation reactions was thermodynamically favorable and the conversion rate reached 81%. The mannose production using whole-cell biocatalysts reached 75.4 g/L in a 30-L reactor, indicating the potential industrial application. Furthermore, the produced mannose in the reactor was directly served as feedstock for the fermentation process to bottom-up produced 19.2 g/L mannosyl-oligosaccharides (MOS) and 7.2 g/L mannosylglycerate (MG) using recombinant Corynebacterium glutamicum strains. Notably, such a mannose fermentation process facilitated the synthesis of MOS, which has not been achieved under glucose fermentation and improved MG production by 2.6-fold than that using the same C-mole of glucose. This approach also allowed access to produce other kinds of mannosyl derivatives from starch.

摘要

淀粉/纤维素因其丰富性和可持续性而成为制造生物燃料和生物化学物质的主要原料。在本研究中,我们通过结合体内和体外代谢工程策略的优势,提出了一种人为设计的“淀粉-甘露糖-发酵”生物转化过程。淀粉最初通过体外代谢工程生物系统转化为甘露糖,然后甘露糖通过工程微生物发酵用于生物制造有价值的甘露糖基化合物。基于磷酸化/去磷酸化反应的体外代谢工程生物系统热力学上是有利的,转化率达到 81%。在 30-L 反应器中,使用全细胞生物催化剂生产的甘露糖产量达到 75.4 g/L,表明具有潜在的工业应用前景。此外,在反应器中生产的甘露糖可直接作为发酵过程的原料,使用重组谷氨酸棒状杆菌菌株从下到上生产 19.2 g/L 甘露糖低聚糖(MOS)和 7.2 g/L 甘露糖甘油酸(MG)。值得注意的是,这种甘露糖发酵工艺有利于合成 MOS,在葡萄糖发酵中无法实现,并且比使用相同的 C-摩尔葡萄糖提高了 2.6 倍的 MG 产量。该方法还允许从淀粉生产其他种类的甘露糖衍生物。

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