Structural determinants and hydrogen-bond network of the mononuclear zinc(II)-beta-lactamase active site

Zinc(II)-beta-lactamases are among the latest generation of antibiotic-resistant enzymes developed by bacteria against beta-lactams. Here we have used density functional theory to provide the full structure of the catalytic site from Bacillus cereus mononuclear beta-lactamase II. Calculations are carried out on relative large models built on the X-ray structure of the free enzyme at the highest available resolution (1.7 A, PDB entry 3BC2). The most stable conformation emerging from our calculations consists of a Zn(II)-bound hydroxide, which acts as nucleophilic agent in the enzymatic reaction, highly stabilized by a complex hydrogen-bond network, in which the protonation state of Asp90 plays a major role. The pattern differs from that previously proposed on the basis of smaller models. Furthermore, the calculations confirm that Arg91 contributes to determine the orientation and the protonation state of Asp90, as recently suggested by mutagenesis experiments.

Structural determinants and hydrogen-bond network of the mononuclear zinc(II)-beta-lactamase active site

Optimal enzyme utilization suggests that concentrations and thermodynamics determine binding mechanisms and enzyme saturations

Seasonal and spatial variability of antibiotic resistance genes and Class I integrons in the rivers of the Mekong delta, Vietnam

Multihole water oxidation catalysis on haematite photoanodes revealed by operando spectroelectrochemistry and DFT

Seasonal and spatial variability of antibiotic resistance genes and Class I integrons in the rivers of the Mekong delta, Vietnam

Optimal enzyme utilization suggests that concentrations and thermodynamics determine binding mechanisms and enzyme saturations

Multihole water oxidation catalysis on haematite photoanodes revealed by operando spectroelectrochemistry and DFT