Discovery and optimisation of potent, selective, ethanolamine inhibitors of bacterial phenylalanyl tRNA synthetase

Richard Lewis Jarvest,Symon G. Erskine,Andrew Keith Forrest,Andrew Fosberry,Martin Hibbs,Joanna J. Jones,Peter J. O'Hanlon,Robert J. Sheppard,Angela Worby

Discovery and optimisation of potent, selective, ethanolamine inhibitors of bacterial phenylalanyl tRNA synthetase

2005

Richard Lewis Jarvest
Symon G. Erskine
Andrew Keith Forrest
Andrew Fosberry
Martin Hibbs
Joanna J. Jones
Peter J. O'Hanlon
Robert J. Sheppard
Angela Worby

High throughput screening of Staphylococcus aureus phenylalanyl tRNA synthetase (FRS) identified ethanolamine 1 as a sub-micromolar hit. Optimisation studies led to the enantiospecific lead 64, a single-figure nanomolar inhibitor. The inhibitor series shows selectivity with respect to the mammalian enzyme and the potential for broad spectrum bacterial FRS inhibition.

Keywords:

Phenylalanine—tRNA ligase
Ethanolamine
Chemical synthesis
Staphylococcus aureus
Enzyme
High-throughput screening
Organic chemistry
Chemistry
Stereochemistry
Enzyme inhibitor
In vitro
Biochemistry
antibacterial agent
Structure–activity relationship

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