Development of autotaxin inhibitors: A series of tetrazole cinnamides.

Christopher Thomson,Darren Mark Le Grand,Mark R. Dowling,David Beattie,Lucy Elphick,Michael Faller,Mark Freeman,Elizabeth Hardaker,Victoria Head,Rene Hemmig,Johan C. Hill,Andrew Lister,David D. Pascoe,S. Rieffel,Binesh Shrestha,Oliver Ross Steward,Florence Zink

Development of autotaxin inhibitors: A series of tetrazole cinnamides.

2020

Christopher Thomson
Darren Mark Le Grand
Mark R. Dowling
David Beattie
Lucy Elphick
Michael Faller
Mark Freeman
Elizabeth Hardaker
Victoria Head
Rene Hemmig
Johan C. Hill
Andrew Lister
David D. Pascoe
S. Rieffel
Binesh Shrestha
Oliver Ross Steward
Florence Zink

Abstract A series of inhibitors of Autotaxin (ATX) have been developed from a high throughput screening hit, 1a, which shows an alternative binding mode to known catalytic site inhibitors. Selectivity over the hERG channel and microsomal clearance were dependent on the lipophilicity of the compounds, and this was optimised by reduction of clogD whilst maintaining high affinity ATX inhibition. Compound 15a shows good oral exposure, and concentration dependent inhibition of formation of LPA in vivo, as shown in pharmacokinetic-pharmacodynamic (PK/PD) experiments.

Keywords:

hERG
PK/PD models
Lipophilicity
Microsome
Combinatorial chemistry
In vivo
Chemistry
Autotaxin
Selectivity
Tetrazole

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