Your search keyword '"Luxenburger, Eva"' showing total 2 results

1. AibA/AibB Induces an Intramolecular Decarboxylation in Isovalerate Biosynthesis by Myxococcus xanthus.

Author

Bock, Tobias, Luxenburger, Eva, Hoffmann, Judith, Schütza, Vlad, Feiler, Christian, Müller, Rolf, and Blankenfeldt, Wulf

Subjects

*DECARBOXYLATION, *COENZYMES, *BIOSYNTHESIS, *MYXOCOCCUS xanthus, *CRYSTAL structure, *SYNTHETIC biology

Abstract

Isovaleryl coenzyme A (IV-CoA) is an important precursor for iso-fatty acids and lipids. It acts in the development of myxobacteria, which can produce this compound from acetyl-CoA through alternative IV-CoA biosynthesis (aib). A central reaction of aib is catalyzed by AibA/AibB, which acts as a cofactor-free decarboxylase despite belonging to the family of CoA-transferases. We developed an efficient expression system for AibA/AibB that allowed the determination of high-resolution crystal structures in complex with different ligands. Through mutational studies, we show that an active-site cysteine previously proposed to be involved in decarboxylation is not required for activity. Instead, AibA/AibB seems to induce an intramolecular decarboxylation by binding its substrate in a hydrophobic cavity and forcing it into a bent conformation. Our study opens opportunities for synthetic biology studies, since AibA/AibB may be suitable for the production of isobutene, a precursor of biofuels and chemicals. [ABSTRACT FROM AUTHOR]

Published

2017

2. Heterologous production of myxobacterial α-pyrone antibiotics in Myxococcus xanthus.

Author

Sucipto, Hilda, Pogorevc, Domen, Luxenburger, Eva, Wenzel, Silke C., and Müller, Rolf

Subjects

*MYXOBACTERALES, *MYXOCOCCUS xanthus, *RNA polymerases, *RIFAMPIN, *ANTIBACTERIAL agents

Abstract

Myxopyronins (MXN) and corallopyronins (COR) are structurally related α-pyrone antibiotics from myxobacteria that represent a highly promising compound class for the development of broad-spectrum antibacterial therapeutic agents. Their ability to inhibit RNA polymerase through interaction with the “switch region”, a novel target, distant from previously characterized RNA polymerase inhibitors (e.g. rifampicin), makes them particularly promising candidates for further research. To improve compound supply for further investigation of MXN, COR and novel derivatives of these antibacterial agents, establishment of an efficient and versatile microbial production platform for myxobacterial α-pyrone antibiotics is highly desirable. Here we describe design, construction and expression of a heterologous production and engineering platforms for MXN and COR to facilitate rational structure design and yield improvement approaches in the myxobacterial host strain Myxococcus xanthus DK1622. Optimization of the cultivation medium yielded significantly higher production titers of MXN A at around 41-fold increase and COR A at around 25-fold increase, compared to the standard CTT medium. [ABSTRACT FROM AUTHOR]

Published

2017