The Interaction of Beta-Lactam Compounds with Chromosomally Mediated Enzymes: Relations to the Molecular Structure
- 1 January 1985
- journal article
- research article
- Published by S. Karger AG in Chemotherapy
- Vol. 31 (4) , 272-278
- https://doi.org/10.1159/000238347
Abstract
The interaction of 25 β-lactam compounds with both chromosomally mediated β-lactamases from Enterobacter cloacae and Citrobacter freundii was studied by enzyme kinetics. All the penams, cephems, and the penem Sch 29482 revealed ‘competitive inhibition’ of both enzymes. The penem required a preincubation period of approximately 5 min before reaching a state of equilibrium between the active and the inactive enzyme. Except for the recently developed compound HR 810, newer cephalosporins generally exhibited a high affinity for both enzymes. Consistent with earlier findings la-tamoxef, N-formimidoyl thienamycin, aztreonam and clavulanic acid showed a time dependent inhibition of the enzyme activity. These findings suggest a more complex reaction scheme including a second reversible complex. The last-mentioned compounds share one structural property: the modification or even the loss of the ring fused to the β-lactam ring. Among these compounds, clavulanic acid exhibited the lowest affinity for the enzymes. It seems likely that the affinity of β-lactam compounds is mainly influenced by the nature of the substituents.Keywords
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