Design, synthesis and biological evaluation of potent NAD+-dependent DNA ligase inhibitors as potential antibacterial agents. Part I: Aminoalkoxypyrimidine carboxamides

Wenxin Gu,Tiansheng Wang,Francois Maltais,Brian Ledford,Joseph M. Kennedy,Yunyi Wei,Christian H. Gross,Jonathan D. Parsons,Leonard R. Duncan,S.J. Ryan Arends,Cameron Stuver Moody,Emanuele Perola,Jeremy Green,Paul S. Charifson

Design, synthesis and biological evaluation of potent NAD+-dependent DNA ligase inhibitors as potential antibacterial agents. Part I: Aminoalkoxypyrimidine carboxamides

2012

Wenxin Gu
Tiansheng Wang
Francois Maltais
Brian Ledford
Joseph M. Kennedy
Yunyi Wei
Christian H. Gross
Jonathan D. Parsons
Leonard R. Duncan
S.J. Ryan Arends
Cameron Stuver Moody
Emanuele Perola
Jeremy Green
Paul S. Charifson

Abstract A series of 2,6-disubstituted aminoalkoxypyrimidine carboxamides (AAPCs) with potent inhibition of bacterial NAD + -dependent DNA ligase was discovered through the use of structure-guided design. Two subsites in the NAD + -binding pocket were explored to modulate enzyme inhibitory potency: a hydrophobic selectivity region was explored through a series of 2-alkoxy substituents while the sugar (ribose) binding region of NAD + was explored via 6-alkoxy substituents.

Keywords:

Enzyme
Ribose
DNA ligase
Potency
Molecular biology
Biochemistry
Chemistry
NAD+ kinase
design synthesis
biological evaluation
nad dependent
Stereochemistry
Selectivity

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