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Potent Triazolopyridine Myeloperoxidase Inhibitors.

ACS medicinal chemistry letters(2018)

Cited 20|Views41
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Abstract
Myeloperoxidase (MPO) generates reactive oxygen species that potentially contribute to many chronic inflammatory diseases. A recently reported triazolopyrimidine MPO inhibitor was optimized to improve acid stability and remove methyl guanine methyl transferase (MGMT) activity. Multiple synthetic routes were explored that allowed rapid optimization of a key benzyl ether side chain. Crystal structures of inhibitors bound to the MPO active site demonstrated alternate binding modes and guided rational design of MPO inhibitors. Thioether showed significant inhibition of MPO activity in an acute mouse inflammation model after oral dosing.
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Key words
Myeloperoxidase,peroxidase,methyl guanine methyl transferase,X-ray crystallography,lead optimization
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