Author:
Milo Scarlet,Heylen Rachel A.,Glancy John,Williams George T.,Patenall Bethany L.,Hathaway Hollie J.,Thet Naing T.,Allinson Sarah L.,Laabei Maisem,Jenkins A. Toby A.
Abstract
AbstractInfection and blockage of indwelling urinary catheters is significant owing to its high incidence rate and severe medical consequences. Bacterial enzymes are employed as targets for small molecular intervention in human bacterial infections. Urease is a metalloenzyme known to play a crucial role in the pathogenesis and virulence of catheter-associated Proteus mirabilis infection. Targeting urease as a therapeutic candidate facilitates the disarming of bacterial virulence without affecting bacterial fitness, thereby limiting the selective pressure placed on the invading population and lowering the rate at which it will acquire resistance. We describe the design, synthesis, and in vitro evaluation of the small molecular enzyme inhibitor 2-mercaptoacetamide (2-MA), which can prevent encrustation and blockage of urinary catheters in a physiologically representative in vitro model of the catheterized urinary tract. 2-MA is a structural analogue of urea, showing promising competitive activity against urease. In silico docking experiments demonstrated 2-MA’s competitive inhibition, whilst further quantum level modelling suggests two possible binding mechanisms.
Funder
Annette Trust
Engineering and Physical Sciences Research Council
University of Kent, GCDC
James Tudor Foundation
Publisher
Springer Science and Business Media LLC
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