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通过优化细胞色素P450 CYP97H1活性在[具体对象]中生产β-隐黄质

β-Cryptoxanthin Production in by Optimization of the Cytochrome P450 CYP97H1 Activity.

作者信息

Lautier Thomas, Smith Derek J, Yang Lay Kien, Chen Xixian, Zhang Congqiang, Truan Gilles, Lindley Nic D

机构信息

Singapore Institute of Food and Biotechnology Innovation (SIFBI), Agency for Science, Technology and Research (A*STAR), 138669 Singapore.

TBI, Université de Toulouse, CNRS, INRAE, INSA, 31077 Toulouse, France.

出版信息

J Agric Food Chem. 2023 Mar 22;71(11):4683-4695. doi: 10.1021/acs.jafc.2c08970. Epub 2023 Mar 8.

Abstract

Cytochromes P450, forming a superfamily of monooxygenases containing heme as a cofactor, show great versatility in substrate specificity. Metabolic engineering can take advantage of this feature to unlock novel metabolic pathways. However, the cytochromes P450 often show difficulty being expressed in a heterologous chassis. As a case study in the prokaryotic host , the heterologous synthesis of β-cryptoxanthin was addressed. This carotenoid intermediate is difficult to produce, as its synthesis requires a monoterminal hydroxylation of β-carotene whereas most of the classic carotene hydroxylases are dihydroxylases. This study was focused on the optimization of the activity of CYP97H1, an original P450 β-carotene monohydroxylase. Engineering the N-terminal part of CYP97H1, identifying the matching redox partners, defining the optimal cellular background and adjusting the culture and induction conditions improved the production by 400 times compared to that of the initial strain, representing 2.7 mg/L β-cryptoxanthin and 20% of the total carotenoids produced.

摘要

细胞色素P450构成了一个以血红素作为辅因子的单加氧酶超家族,在底物特异性方面表现出极大的多样性。代谢工程可以利用这一特性来开启新的代谢途径。然而,细胞色素P450在异源宿主中往往难以表达。作为原核宿主中的一个案例研究,探讨了β-隐黄质的异源合成。这种类胡萝卜素中间体难以生产,因为其合成需要β-胡萝卜素的单末端羟基化,而大多数经典的胡萝卜素羟化酶是双羟化酶。本研究聚焦于优化CYP97H1(一种原始的P450β-胡萝卜素单加氧酶)的活性。对CYP97H1的N端部分进行工程改造、确定匹配的氧化还原伙伴、定义最佳细胞背景并调整培养和诱导条件,与初始菌株相比,产量提高了400倍,达到2.7mg/L的β-隐黄质,占总类胡萝卜素产量的20%。

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