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Cofactor Regeneration by a Soluble Pyridine Nucleotide Transhydrogenase for Biological Production of Hydromorphone

机译:可溶性吡啶核苷酸转氢酶的辅因子再生用于生物产生氢吗啡酮

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We have applied the soluble pyridine nucleotide transhydrogenase ofPseudomonas fluorescens to a cell-free system for the regeneration of the nicotinamide cofactors NAD and NADP in the biological production of the important semisynthetic opiate drug hydromorphone. The original recombinant whole-cell system suffered from cofactor depletion resulting from the action of an NADP+-dependent morphine dehydrogenase and an NADH-dependent morphinone reductase. By applying a soluble pyridine nucleotide transhydrogenase, which can transfer reducing equivalents between NAD and NADP, we demonstrate with a cell-free system that efficient cofactor cycling in the presence of catalytic amounts of cofactors occurs, resulting in high yields of hydromorphone. The ratio of morphine dehydrogenase, morphinone reductase, and soluble pyridine nucleotide transhydrogenase is critical for diminishing the production of the unwanted by-product dihydromorphine and for optimum hydromorphone yields. Application of the soluble pyridine nucleotide transhydrogenase to the whole-cell system resulted in an improved biocatalyst with an extended lifetime. These results demonstrate the usefulness of the soluble pyridine nucleotide transhydrogenase and its wider application as a tool in metabolic engineering and biocatalysis.
机译:我们已将荧光假单胞菌的可溶性吡啶核苷酸转氢酶应用于无细胞系统,以在重要的半合成阿片类药物氢吗啡酮的生物生产中再生烟酰胺辅因子NAD和NADP。最初的重组全细胞系统由于依赖于NADP + 的吗啡脱氢酶和依赖NADH的吗啡酮还原酶而遭受辅因子的消耗。通过应用可在NAD和NADP之间转移还原当量的可溶性吡啶核苷酸转氢酶,我们用无细胞系统证明了在催化量的辅因子存在下有效的辅因子循环发生,从而导致氢吗啡酮的高收率。吗啡脱氢酶,吗啡酮还原酶和可溶性吡啶核苷酸转氢酶的比例对于减少不需要的副产物二氢吗啡的产量和最佳氢吗啡酮产量至关重要。可溶性吡啶核苷酸转氢酶在全细胞系统中的应用导致了生物催化剂的改进,使用寿命延长。这些结果证明了可溶性吡啶核苷酸转氢酶的有用性及其作为代谢工程和生物催化工具的广泛应用。

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