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Enhancing solubility of deoxyxylulose phosphate pathway enzymes for microbial isoprenoid production

机译:增强脱氧木酮糖磷酸途径酶在微生物类异戊二烯产生中的溶解度

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摘要

Background:Recombinant proteins are routinely overexpressed in metabolic engineering. It is well known that some over-expressed heterologous recombinant enzymes are insoluble with little or no enzymatic activity. This study examined the solubility of over-expressed homologous enzymes of the deoxyxylulose phosphate pathway (DXP) and the impact of inclusion body formation on metabolic engineering of microbes.Results:Four enzymes of this pathway (DXS, ISPG, ISPH and ISPA), but not all, were highly insoluble, regardless of the expression systems used. Insoluble dxs (the committed enzyme of DXP pathway) was found to be inactive. Expressions of fusion tags did not significantly improve the solubility of dxs. However, hypertonic media containing sorbitol, an osmolyte, successfully doubled the solubility of dxs, with the concomitant improvement in microbial production of the metabolite, DXP. Similarly, sorbitol significantly improved the production of soluble and functional ERG12, the committed enzyme in the mevalonate pathway.Conclusion:This study demonstrated the unanticipated findings that some over-expressed homologous enzymes of the DXP pathway were highly insoluble, forming inclusion bodies, which affected metabolite formation. Sorbitol was found to increase both the solubility and function of some of these over-expressed enzymes, a strategy to increase the production of secondary metabolites.
机译:背景:重组蛋白在代谢工程中通常过表达。众所周知,一些过表达的异源重组酶是不溶的,几乎没有酶活性。这项研究检查了过表达的脱氧木酮糖磷酸途径(DXP)的同源酶的溶解度以及包涵体形成对微生物代谢工程的影响。结果:该途径的四种酶(DXS,ISPG,ISPH和ISPA)并非全部,都是高度不溶的,无论使用哪种表达系统。发现不溶性dxs(DXP途径的定型酶)没有活性。融合标签的表达并未显着改善dxs的溶解度。但是,含有山梨糖醇(一种渗透压剂)的高渗介质成功地使dxs的溶解度增加了一倍,并伴随着代谢物DXP的微生物产生的改善。同样,山梨糖醇显着提高了甲羟戊酸途径中固定酶的可溶性和功能性ERG12的生成。代谢物的形成。发现山梨糖醇可增加某些这些过表达酶的溶解度和功能,这是增加次级代谢产物产生的一种策略。

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