Highly Selective Sub-Nanomolar Cathepsin S Inhibitors by Merging Fragment Binders with Nitrile Inhibitors.

Markus Schade Beatrix Merla Bernhard Lesch Markus Wagener Simone Timmermanns Katrien Pletinckx Torsten Hertrampf

Published in: Journal of medicinal chemistry (2020)

Pharmacological inhibition of cathepsin S (CatS) allows for a specific modulation of the adaptive immune system and many major diseases. Here, we used NMR fragment screening and crystal structure-aided merging to synthesize novel, highly selective CatS inhibitors with picomolar enzymatic Ki values and nanomolar functional activity in human Raji cells. Noncovalent fragment hits revealed binding hotspots, while the covalent inhibitor structure-activity relationship enabled efficient potency optimization.

Keyphrases

crystal structure
structure activity relationship
induced apoptosis
endothelial cells
magnetic resonance
high resolution
hydrogen peroxide
single cell
oxidative stress
squamous cell carcinoma
induced pluripotent stem cells
signaling pathway
pluripotent stem cells
mass spectrometry
binding protein
rectal cancer