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Biosynthesis of Menaquinone (Vitamin K2) and Ubiquinone (Coenzyme Q).

机译:甲基萘醌(维生素K2)和泛醌(辅酶Q)的生物合成。

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摘要

Escherichia coli and Salmonella contain the naphthoquinones menaquinone (MK; vitamin K2) and demethylmenaquinone and the benzoquinone ubiquinone (coenzyme Q; Q). Both quinones are derived from the shikimate pathway, which has been called a "metabolic tree with many branches." There are two different pathways for the biosynthesis of the naphthoquinones. The vast majority of prokaryotes, including E. coli and Salmonella, and the plants use the o-succinylbenzoate pathway, while a minority uses the futalosine pathway. The quinone nucleus of Q is derived directly from chorismate, while that of MK is derived from chorismate via isochorismate. The prenyl side chains of both quinones are from isopentenyl diphosphate formed by the 2-C-methyl-D-erythritol 4-phosphate (non-mevalonate) pathway and the methyl groups are from S-adenosylmethionine. In addition, MK biosynthesis requires 2-ketoglutarate and cofactors ATP, coenzyme A, and thiamine pyrophosphate. Despite the fact that both quinones originate from the shikimate pathway, there are important differences in their biosyntheses. The prenyl side chain in MK biosynthesis is introduced at the penultimate step, accompanied by decarboxylation, whereas in Q biosynthesis it is introduced at the second step, with retention of the carboxyl group. In MK biosynthesis, all the reactions of the pathway up to prenylation are carried out by soluble enzymes, whereas all the enzymes involved in Q biosynthesis except the first are membrane bound. In MK biosynthesis, the last step is a C-methylation; in Q biosynthesis, the last step is an O-methylation. In Q biosynthesis a second C-methylation and O-methylation take place in the middle part of the pathway. Despite the fact that Q and MK biosyntheses diverge at chorismate, the C-methylations in both pathways are carried out by the same methyltransferase.
机译:大肠杆菌和沙门氏菌含有萘醌甲萘醌(MK;维生素K2),去甲基甲萘醌和苯醌泛醌(辅酶Q; Q)。两种醌均源自the草酸途径,该途径被称为“具有许多分支的代谢树”。萘醌的生物合成有两种不同的途径。绝大多数的原核生物,包括大肠杆菌和沙门氏菌,以及植物都使用邻琥珀酰苯甲酸酯途径,而少数则使用了他他洛辛途径。 Q的醌核直接来自分支酸,而MK的醌核则来自异氰酸酯的分支酸。两个醌的异戊烯基侧链均来自通过2-C-甲基-D-赤藓糖醇4-磷酸(非甲羟戊酸)途径形成的异戊烯基二磷酸,并且甲基来自S-腺苷甲硫氨酸。此外,MK生物合成需要2-酮戊二酸和辅助因子ATP,辅酶A和硫胺素焦磷酸。尽管两个醌均源自sh草酸酯途径,但它们的生物合成存在重要差异。在MK生物合成中,异戊二烯侧链在倒数第二步引入,并伴随脱羧作用;而在Q生物合成中,异戊二烯侧链在第二步引入,并保留羧基。在MK生物合成中,直至异戊二烯化的途径的所有反应均由可溶性酶完成,而Q生物合成中除第一个酶外的所有酶都是膜结合的。在MK生物合成中,最后一步是C-甲基化。在Q生物合成中,最后一步是O-甲基化。在Q生物合成中,第二C-甲基化和O-甲基化发生在途径的中间部分。尽管Q和MK的生物合成在分支酸上存在差异,但两种途径中的C-甲基化是由相同的甲基转移酶进行的。

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    Meganathan R.; Kwon Ohsuk;

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  • 年度 2009
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