Optimisation of aryl substitution leading to potent methionyl tRNA synthetase inhibitors with excellent gram-positive antibacterial activity

Richard Lewis Jarvest,John Michael Berge,Murray J.B. Brown,Pamela Brown,John Stephen Elder,Andrew Keith Forrest,Catherine S. V. Houge-Frydrych,Peter J. O'Hanlon,David J McNair,Stephen Rittenhouse,Robert J. Sheppard

Optimisation of aryl substitution leading to potent methionyl tRNA synthetase inhibitors with excellent gram-positive antibacterial activity

2003

Richard Lewis Jarvest
John Michael Berge
Murray J.B. Brown
Pamela Brown
John Stephen Elder
Andrew Keith Forrest
Catherine S. V. Houge-Frydrych
Peter J. O'Hanlon
David J McNair
Stephen Rittenhouse
Robert J. Sheppard

Optimisation of the left-hand-side aryl moiety of a file compound screening hit against Staphylococcus aureus methionyl tRNA synthetase led to the identification of a series of potent nanomolar inhibitors. The best compounds showed excellent antibacterial activity against staphylococcal and enterococcal pathogens, including strains resistant to clinical antibiotics.

Keywords:

Staphylococcus epidermidis
Organic chemistry
Staphylococcus aureus
Aryl
Moiety
Gram-positive bacteria
Biochemistry
Stereochemistry
Antibiotics
Antibacterial activity
Chemistry
Bacteria
antibacterial agent

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