Angewandte Chemie - International Edition, volume 63, issue 38

Structural Elucidation of a Metagenomic Urethanase and Its Engineering Towards Enhanced Hydrolysis Profiles

Thomas Bayer 1
Gottfried J. Palm 2
Leona Berndt 2
Hannes Meinert 1
Yannick Branson 1
Louis Schmidt 3
Clemens Cziegler 1
Ina Somvilla 1, 4
Celine Zurr 1
Leonie G Graf 2, 4
Una Janke 5, 6
Christoffel P. S. Badenhorst 1
Stefanie König 3
Mihaela Delcea 6, 7
Ulrike Garscha 3
Ren Wei 1
Michael Lammers 2
Show full list: 18 authors
Publication typeJournal Article
Publication date2024-08-16
scimago Q1
SJR5.300
CiteScore26.6
Impact factor16.1
ISSN14337851, 15213773
Abstract

While plastics like polyethylene terephthalate can already be degraded efficiently by the activity of hydrolases, other synthetic polymers like polyurethanes (PUs) and polyamides (PAs) largely resist biodegradation. In this study, we solved the first crystal structure of the metagenomic urethanase UMG‐SP‐1, identified highly flexible loop regions to comprise active site residues, and targeted a total of 20 potential hot spots by site‐saturation mutagenesis. Engineering campaigns yielded variants with single mutations, exhibiting almost 3‐ and 8‐fold improved activity against highly stable N‐aryl urethane and amide bonds, respectively. Furthermore, we demonstrated the release of the corresponding monomers from a thermoplastic polyester‐PU and a PA (nylon 6) by the activity of a single, metagenome‐derived urethanase after short incubation times. Thereby, we expanded the hydrolysis profile of UMG‐SP‐1 beyond the reported low‐molecular weight carbamates. Together, these findings promise advanced strategies for the bio‐based degradation and recycling of plastic materials and waste, aiding efforts to establish a circular economy for synthetic polymers.

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