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从茶园土壤中分离出的耐咖啡因细菌CT25中,各种甲基黄嘌呤触发的不同分解代谢途径

Different Catabolism Pathways Triggered by Various Methylxanthines in Caffeine-Tolerant Bacterium CT25 Isolated from Tea Garden Soil.

作者信息

Ma Yi-Xiao, Wu Xiao-Han, Wu Hui-Shi, Dong Zhan-Bo, Ye Jian-Hui, Zheng Xin-Qiang, Liang Yue-Rong, Lu Jianliang

机构信息

Zhejiang University Tea Research Institute, Hangzhou 310058, P.R. China.

Chongqing Vocational College of Transportation, Chongqing 402247, P.R. China.

出版信息

J Microbiol Biotechnol. 2018 Jul 28;28(7):1147-1155. doi: 10.4014/jmb.1801.01043.

Abstract

The degradation efficiency and catabolism pathways of the different methylxanthines (MXs) in isolated caffeine-tolerant strain CT25 were comprehensively studied. The results showed that the degradation efficiency of various MXs varied with the number and position of the methyl groups on the molecule (, xanthine > 7-methylxanthine ≈ theobromine > caffeine > theophylline > 1-methylxanthine). Multiple MX catabolism pathways coexisted in strain CT25, and a different pathway would be triggered by various MXs. Demethylation dominated in the degradation of N-7-methylated MXs (such as 7-methylxanthine, theobromine, and caffeine), where C-8 oxidation was the major pathway in the catabolism of 1-methylxanthine, whereas demethylation and C-8 oxidation are likely both involved in the degradation of theophylline. Enzymes responsible for MX degradation were located inside the cell. Both cell culture and cell-free enzyme assays revealed that N-1 demethylation might be a rate-limiting step for the catabolism of the MXs. Surprisingly, accumulation of uric acid was observed in a cell-free reaction system, which might be attributed to the lack of activity of uricase, a cytochrome -coupled membrane integral enzyme.

摘要

对分离出的耐咖啡因菌株CT25中不同甲基黄嘌呤(MXs)的降解效率和分解代谢途径进行了全面研究。结果表明,各种MXs的降解效率随分子上甲基的数量和位置而变化(, 黄嘌呤>7-甲基黄嘌呤≈可可碱>咖啡因>茶碱>1-甲基黄嘌呤)。菌株CT25中存在多种MX分解代谢途径,不同的MX会触发不同的途径。N-7-甲基化MXs(如7-甲基黄嘌呤、可可碱和咖啡因)的降解以去甲基化为主,其中C-8氧化是1-甲基黄嘌呤分解代谢的主要途径,而茶碱的降解可能涉及去甲基化和C-8氧化。负责MX降解的酶位于细胞内。细胞培养和无细胞酶分析均表明,N-1去甲基化可能是MXs分解代谢的限速步骤。令人惊讶的是,在无细胞反应体系中观察到尿酸的积累,这可能归因于细胞色素偶联膜整合酶尿酸酶活性的缺乏。

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