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Biosynthesis of Ubiquinone Compounds with Conjugated Prenyl Side Chains

机译:带有共轭异戊二烯侧链的泛醌化合物的生物合成

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Enzymatic steps from two different biosynthetic pathways were combined in Escherichia coli, directing the synthesis of a new class of biomolecules—ubiquinones with prenyl side chains containing conjugated double bonds. This was achieved by the activity of a C30 carotenoid desaturase, CrtN, from Staphylococcus aureus, which exhibited an inherent flexibility in substrate recognition compared to other carotenoid desaturases. By utilizing the known plasticity of E. coli's native ubiquinone biosynthesis pathway and the unusual activity of CrtN, modified ubiquinone structures with prenyl side chains containing conjugated double bonds were generated. The side chains of the new structures were confirmed to have different degrees of desaturation by mass spectrometry and nuclear magnetic resonance analysis. In vivo 14C labeling and in vitro activity studies showed that CrtN desaturates octaprenyl diphosphates but not the ubiquinone compounds directly. Antioxidant properties of conjugated side chain ubiquinones were analyzed in an in vitro β-carotene-linoleate model system and were found to be higher than the corresponding unmodified ubiquinones. These results demonstrate that by combining pathway steps from different branches of biosynthetic networks, classes of compounds not observed in nature can be synthesized and structural motifs that are functionally important can be combined or enhanced.
机译:来自两种不同生物合成途径的酶促步骤在大肠杆菌中结合在一起,指导了新一类生物分子的合成-带有异戊二烯侧链的共轭双键泛醌。这是通过金黄色葡萄球菌的C30类胡萝卜素去饱和酶CrtN的活性实现的,与其他类胡萝卜素去饱和酶相比,该酶在底物识别方面表现出固有的灵活性。通过利用大肠杆菌天然的泛醌生物合成途径的已知可塑性和CrtN的异常活性,产生了带有含有共轭双键的异戊二烯侧链的修饰泛醌结构。质谱和核磁共振分析证实新结构的侧链具有不同的去饱和度。体内14C标记和体外活性研究表明,CrtN使辛二烯基二磷酸酯不饱和,而直接使泛醌化合物不饱和。在体外β-胡萝卜素-亚油酸酯模型系统中分析了共轭侧链泛醌的抗氧化性能,发现其比相应的未修饰泛醌要高。这些结果表明,通过组合来自生物合成网络不同分支的途径步骤,可以合成自然界中未观察到的化合物类别,并且可以组合或增强功能上重要的结构基序。

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