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Title: The Zn2 Position in Metallo-beta-Lactamases is Critical for Activity: A Study on Chimeric Metal Sites on a Conserved Protein Scaffold

Journal Article · · Journal of Molecular Biology

Metallo-?-lactamases (M?Ls) are bacterial Zn(II)-dependent hydrolases that confer broad-spectrum resistance to ?-lactam antibiotics. These enzymes can be subdivided into three subclasses (B1, B2 and B3) that differ in their metal binding sites and their characteristic tertiary structure. To date there are no clinically useful pan-M?L inhibitors available, mainly due to the unawareness of key catalytic features common to all M?L brands. Here we have designed, expressed and characterized two double mutants of BcII, a di-Zn(II) B1-M?L from Bacillus cereus, namely BcII-R121H/C221D (BcII-HD) and BcII-R121H/C221S (BcII-HS). These mutants display modified environments at the so-called Zn2 site or DCH site, reproducing the metal coordination environments of structurally related metallohydrolases. Through a combination of structural and functional studies, we found that BcII-HD is an impaired ?-lactamase even as a di-Zn(II) enzyme, whereas BcII-HS exhibits the ability to exist as mono or di-Zn(II) species in solution, with different catalytic performances. We show that these effects result from an altered position of Zn2, which is incapable of providing a productive interaction with the substrate ?-lactam ring. These results indicate that the position of Zn2 is essential for a productive substrate binding and hydrolysis.

Research Organization:
Brookhaven National Lab. (BNL), Upton, NY (United States). National Synchrotron Light Source
Sponsoring Organization:
Doe - Office Of Science
DOE Contract Number:
DE-AC02-98CH10886
OSTI ID:
959736
Report Number(s):
BNL-82722-2009-JA; JMOBAK; TRN: US201016%%880
Journal Information:
Journal of Molecular Biology, Vol. 373; ISSN 0022-2836
Country of Publication:
United States
Language:
English