Positioning of an unprecedented spiro[5.5]undeca ring system into kinase inhibitor space.
Arramshetti VenkannaLalita SubediMahesh K TeliPrema Dhorma LamaBhargav Gupta NangunuriSang-Yoon LeeSun Yeou KimMi-Hyun KimPublished in: Scientific reports (2020)
In-house 1,5-oxaza spiroquinone 1, with spiro[5.5]undeca ring system, was announced as an unprecedented anti-inflammatory scaffold through chemistry-oriented synthesis (ChOS), a chemocentric approach. Herein, we studied how to best position the spiro[5.5]undeca ring system in kinase inhibitor space. Notably, late-stage modification of the scaffold 1 into compounds 2a-r enhanced kinase-likeness of the scaffold 1. The improvement could be depicted with (1) selectivity with target shift (from JNK-1 into GSK-3) and (2) potency (>ā20-fold). In addition, ATP independent IC50 of compound 2j suggested a unique binding mode of this scaffold between ATP site and substrate site, which was explained by docking based optimal site selection and molecular dynamic simulations of the optimal binding site. Despite the shift of kinase profiling, the anti-inflammatory activity of compounds 2a-r could be retained in hyperactivated microglial cells.
Keyphrases
- tissue engineering
- induced apoptosis
- signaling pathway
- molecular dynamics
- anti inflammatory
- protein kinase
- tyrosine kinase
- cell cycle arrest
- molecular dynamics simulations
- endoplasmic reticulum stress
- lipopolysaccharide induced
- single cell
- pi k akt
- neuropathic pain
- single molecule
- protein protein
- spinal cord injury
- small molecule
- lps induced
- drug discovery