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中心碳代谢中不为人知的代谢联系。

Unfamiliar metabolic links in the central carbon metabolism.

作者信息

Fuchs Georg, Berg Ivan A

机构信息

Mikrobiologie, Fakultät für Biologie, Universität Freiburg, Schänzlestr. 1, D 79104 Freiburg, Germany.

出版信息

J Biotechnol. 2014 Dec 20;192 Pt B:314-22. doi: 10.1016/j.jbiotec.2014.02.015. Epub 2014 Feb 24.

Abstract

The central carbon metabolism of all organisms is considered to follow a well established fixed scheme. However, recent studies of autotrophic carbon fixation in prokaryotes revealed unfamiliar metabolic links. A new route interconnects acetyl-coenzyme A (CoA) via 3-hydroxypropionate with succinyl-CoA. Succinyl-CoA in turn may be metabolized via 4-hydroxybutyrate to two molecules of acetyl-CoA; a reversal of this route would result in the assimilation of two molecules of acetyl-CoA into C4 compounds. C5-dicarboxylic acids are a rather neglected class of metabolites; yet, they play a key role not only in one of the CO2 fixation cycles, but also in two acetate assimilation pathways that replace the glyoxylate cycle. C5 compounds such as ethylmalonate, methylsuccinate, methylmalate, mesaconate, itaconate and citramalate or their CoA esters are thereby linked to the acetyl-CoA, propionyl-CoA, glyoxylate and pyruvate pools. A novel carboxylase/reductase converts crotonyl-CoA into ethylmalonyl-CoA; similar reductive carboxylations apply to other alpha-beta-unsaturated carboxy-CoA thioesters. These unfamiliar metabolic links may provide useful tools for metabolic engineering.

摘要

所有生物体的中心碳代谢被认为遵循一个既定的固定模式。然而,最近对原核生物中自养碳固定的研究揭示了一些不常见的代谢联系。一条新途径通过3-羟基丙酸将乙酰辅酶A(CoA)与琥珀酰辅酶A连接起来。琥珀酰辅酶A又可以通过4-羟基丁酸代谢为两分子的乙酰辅酶A;这条途径的逆向反应会导致两分子的乙酰辅酶A同化为C4化合物。C5-二羧酸是一类相当被忽视的代谢物;然而,它们不仅在一个二氧化碳固定循环中起关键作用,而且在取代乙醛酸循环的两条乙酸同化途径中也起关键作用。诸如乙基丙二酸、甲基琥珀酸、甲基苹果酸、中康酸、衣康酸和柠康酸等C5化合物或它们的辅酶A酯因此与乙酰辅酶A、丙酰辅酶A、乙醛酸和丙酮酸库相联系。一种新型羧化酶/还原酶将巴豆酰辅酶A转化为乙基丙二酰辅酶A;类似的还原羧化反应也适用于其他α-β-不饱和羧基辅酶A硫酯。这些不常见的代谢联系可能为代谢工程提供有用的工具。

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