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Human metallo-β-lactamase enzymes degrade penicillin.

Sci Rep.. 2019-08; 
Diene SM, Pinault L, Keshri V, Armstrong N, Khelaifia S, Chabrière E, Caetano-Anolles G, Colson P, La Scola B, Rolain JM, Pontarotti P, Raoult D
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Gene Synthesis Genes encoding for human metallo-ß-lactamase enzymes (i.e. LactB2, MBLAC2, SNM1A, and SNMA1B) were optimized for protein expression in Escherichia coli and synthesized by GenScript (Piscataway, NJ, USA). Get A Quote

摘要

Nonribosomal peptides are assemblages, including antibiotics, of canonical amino acids and other molecules. β-lactam antibiotics act on bacterial cell walls and can be cleaved by β-lactamases. β-lactamase activity in humans has been neglected, even though eighteen enzymes have already been annotated such in human genome. Their hydrolysis activities on antibiotics have not been previously investigated. Here, we report that human cells were able to digest penicillin and this activity was inhibited by β-lactamase inhibitor, i.e. sulbactam. Penicillin degradation in human cells was microbiologically demonstrated on Pneumococcus. We expressed a MBLAC2 human β-lactamase, known as an exosome biogenesis enzyme. It... More

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