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Optimization of the Bacterial Cytochrome P450 BM3 System for the Production of Human Drug Metabolites

机译:用于生产人类药物代谢产物的细菌细胞色素P450 BM3系统的优化

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摘要

Drug metabolism in human liver is a process involving many different enzymes. Among them, a number of cytochromes P450 isoforms catalyze the oxidation of most of the drugs commercially available. Each P450 isoform acts on more than one drug, and one drug may be oxidized by more than one enzyme. As a result, multiple products may be obtained from the same drug, and as the metabolites can be biologically active and may cause adverse drug reactions (ADRs), the metabolic profile of a new drug has to be known before this can be commercialized. Therefore, the metabolites of a certain drug must be identified, synthesized and tested for toxicity. Their synthesis must be in sufficient quantities to be used for metabolic tests. This review focuses on the progresses done in the field of the optimization of a bacterial self-sufficient and efficient cytochrome P450, P450 BM3 from Bacillus megaterium, used for the production of metabolites of human enzymes. The progress made in the improvement of its catalytic performance towards drugs, the substitution of the costly NADPH cofactor and its immobilization and scale-up of the process for industrial application are reported.
机译:人肝中的药物代谢是一个涉及许多不同酶的过程。其中,许多细胞色素P450亚型可催化大多数市售药物的氧化。每个P450同工型都作用于一种以上的药物,并且一种药物可能会被一种以上的酶氧化。结果,可以从同一药物中获得多种产品,并且由于代谢物具有生物活性并可能引起药物不良反应(ADR),因此在将新药商业化之前,必须先了解新药的代谢特征。因此,必须鉴定,合成和测试某种药物的代谢物的毒性。它们的合成量必须足够用于代谢测试。这篇综述集中在优化细菌自给自足和高效的细胞色素P450,来自巨大芽孢杆菌的P450 BM3,用于生产人类酶代谢产物方面的进展。据报道,在改善其对药物的催化性能,取代昂贵的NADPH辅因子及其固定化和工业化生产工艺方面取得了进展。

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