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Role of the Conserved Disulfide Bridge in Class A Carbapenemases.

J Biol Chem. 2016; 
Smith CA, Nossoni Z, Toth M, Stewart NK, Frase H, Vakulenko SB.
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PCR Cloning and Subcloning Experimental Procedures Cloning, MIC testing, expression and purification - The genes for the C69G, C69A, C69M and C69L variants of GES-1, GES-2 and GES-5 enzymes and C69G, C69A, C238G and C238A variants of the SME-1, NMCA and SFC-1 carbapenemases along with the C69G/C238G double mutant variants of GES- 5, SME-1 and SFC-1 were custom synthesized (GenScript) with unique NdeI and HindIII restriction sites at the 3’ and 5’ ends, respectively, and cloned into the vector pHF016. Get A Quote

摘要

Some members of the class A β-lactamase family are capable of conferring resistance to the last resort antibiotics, carbapenems. A unique structural feature of these clinically important enzymes, collectively referred to as class A carbapenemases, is a disulfide bridge between invariant Cys69 and Cys238 residues. It was proposed that this conserved disulfide bridge is responsible for their carbapenemase activity, but this has not yet been validated. Here we show that disruption of the disulfide bridge in the GES-5 carbapenemase by the C69G substitution results in only minor decreases in the conferred levels of resistance to the carbapenem imipenem and other β-lactams. Kinetic and circular dichroism experiment... More

关键词

antibiotic resistance; carbapenemase; crystal structure; disulfide; enzyme kinetics; enzyme stability; hydrogen bond