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C4-二羧酸代谢物:大肠杆菌 C4-二羧酸转运蛋白与胞质酶的相互作用。

C4-dicarboxylate metabolons: interaction of C4-dicarboxylate transporters of Escherichia coli with cytosolic enzymes.

机构信息

Institute for Molecular Physiology, Johannes Gutenberg-University, Biozentrum II, Hanns-Dieter-Hüsch-Weg 17, 55128 Mainz, Germany.

Department of Life Science, Ewha Womans University, Seoul 30760, Republic of Korea.

出版信息

FEMS Microbiol Lett. 2022 Sep 22;369(1). doi: 10.1093/femsle/fnac078.

Abstract

Metabolons represent the structural organization of proteins for metabolic or regulatory pathways. Here, the interaction of fumarase FumB, aspartase AspA, and L-tartrate dehydratase TtdAB with the C4-dicarboxylate (C4-DC) transporters DcuA, DcuB, DcuC, and the L-tartrate transporter TtdT of Escherichia coli was tested by a bacterial two-hybrid (BACTH) assay in situ, or by co-chromatography using mSPINE (membrane Streptavidin protein interaction experiment). From the general C4-DC transporters, DcuB interacted with FumB and AspA, DcuA with AspA, whereas DcuC interacted with neither FumB nor AspA. Moreover, TtdT did not interact with TtdAB. The fumB-dcuB, the dcuA-aspA, and the ttdAB-ttdT genes encoding the respective proteins colocalize on the genome and each pair of genes forms cotranscripts, whereas the dcuC gene lies alone. The data suggest the formation of DcuB/FumB and DcuB/AspA metabolons for the uptake of L-malate, or L-aspartate, and their conversion to fumarate for fumarate respiration and excretion of the product succinate. The DcuA/AspA metabolon catalyzes uptake and conversion of L-aspartate to fumarate coupled to succinate excretion. The DcuA/AspA metabolon provides ammonia at the same time for nitrogen assimilation (ammonia shuttle). On the other hand, TtdT and TtdAB are not organized in a metabolon. Reasons for the formation (DcuA/AspA, DcuB/FumB, and DcuB/AspA) or nonformation (DcuC, TtdT, and TtdAB) of metabolons are discussed based on their metabolic roles.

摘要

代谢物代表代谢或调节途径中蛋白质的结构组织。在这里,通过细菌双杂交(BACTH)测定法原位或使用 mSPINE(膜链霉亲和素蛋白相互作用实验)进行共色谱分析,测试了延胡索酸酶 FumB、天冬氨酸酶 AspA 和 L-酒石酸脱水酶 TtdAB 与大肠杆菌的 C4-二羧酸(C4-DC)转运蛋白 DcuA、DcuB、DcuC 和 L-酒石酸转运蛋白 TtdT 的相互作用。从一般的 C4-DC 转运蛋白中,DcuB 与 FumB 和 AspA 相互作用,DcuA 与 AspA 相互作用,而 DcuC 既不与 FumB 也不与 AspA 相互作用。此外,TtdT 与 TtdAB 不相互作用。编码相应蛋白质的 fumB-dcuB、dcuA-aspA 和 ttdAB-ttdT 基因在基因组上共定位,每对基因形成共转录物,而 dcuC 基因则单独存在。这些数据表明,DcuB/FumB 和 DcuB/AspA 代谢物的形成用于摄取 L-苹果酸或 L-天冬氨酸,并将其转化为延胡索酸,用于延胡索酸呼吸和产物琥珀酸的排泄。DcuA/AspA 代谢物催化 L-天冬氨酸摄取和转化为延胡索酸,与琥珀酸排泄偶联。DcuA/AspA 代谢物同时提供氨用于氮同化(氨穿梭)。另一方面,TtdT 和 TtdAB 没有形成代谢物。基于它们的代谢作用,讨论了代谢物形成(DcuA/AspA、DcuB/FumB 和 DcuB/AspA)或不形成(DcuC、TtdT 和 TtdAB)的原因。

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