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Bioorganic Chemistry

Bioorganic Chemistry

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Analysis on benzothiazole necroptosis inhibitors with chiral substitutions in the solvent-accessible region of RIP kinase domain

Published:1 August 2023 DOI: 10.1016/j.bioorg.2023.106647 PMID: 37270986
Hongming Shao , Lijuan Xu , Gechang Li , Shuyu Wang , Ting Han , Chunlin Zhuang

Abstract

Receptor-interacting protein kinase 1 (RIPK1) and RIPK3, two imperative targets of the necroptosis pathway, are associated with various inflammatory-related diseases. Regulating kinase activity with inhibitors has been confirmed as a promising strategy for inflammation treatment. However, most of the reported type I and II kinase inhibitors of RIPK1 and RIPK3, including benzothiazole compounds discovered by our group, have selective limitations due to interaction with ATP-binding pockets. Fortunately, a solvent exposure E0 region of the kinase domain, which extends into the linker region, has been reported to be related to the potency and selectivity of inhibitors. Hence, based on our previous study, a series of benzothiazole necroptosis inhibitors with chiral substitutions in the linker region were developed to investigate RIPK1/3 inhibitory potency. The results showed a 2-to 6-fold increase in anti-necroptotic activity for these chiral compounds. The improved selectivity on RIPK1 or RIPK3 was demonstrated on different derivatives. Predicted binding conformations of enantiomers with RIPK1/3 gave an explanation for their activity differences, guiding further rational design of chiral necroptosis inhibitors.

Substances (4)

Materials
Procduct Name CAS Molecular Formula Supplier Price
Z-Vad-fmk, non-methylated 161401-82-7 C21H28FN3O7 93 suppliers $70.00-$7016.50
Z-Vad-fmk, non-methylated 161401-82-7 C21H28FN3O7 93 suppliers $70.00-$7016.50
Z-Vad-fmk, non-methylated 161401-82-7 C21H28FN3O7 93 suppliers $70.00-$7016.50
Z-Vad-fmk, non-methylated 161401-82-7 C21H28FN3O7 93 suppliers $70.00-$7016.50

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