Subnanomolar Cathepsin S Inhibitors with High Selectivity: Optimizing Covalent Reversible α‐Fluorovinylsulfones and α‐Sulfonates as Potential Immunomodulators in Cancer

Author:

Fuchs Natalie1ORCID,Meta Mergim1ORCID,Lantzberg Bellinda2ORCID,Bros Matthias3ORCID,Ling Kuan Seah2ORCID,Weil Tanja2ORCID,Schirmeister Tanja1ORCID

Affiliation:

1. Institute of Pharmaceutical and Biomedical Sciences (IPBS) Johannes Gutenberg University Mainz Staudingerweg 5 55128 Mainz Germany

2. Max Planck Institute for Polymer Research Ackermannweg 10 55128 Mainz Germany

3. Department of Dermatology University Medical Center Mainz Langenbeckstr. 1 55131 Mainz Germany

Abstract

AbstractThe cysteine protease cathepsin S (CatS) is overexpressed in many tumors. It is known to be involved in tumor progression as well as antigen processing in antigen‐presenting cells (APC). Recent evidence suggests that silencing CatS improves the anti‐tumor immune response in several cancers. Therefore, CatS is an interesting target to modulate the immune response in these diseases. Here, we present a series of covalent‐reversible CatS inhibitors based on the α‐fluorovinylsulfone and ‐sulfonate warheads. We optimized two lead structures by molecular docking approaches, resulting in 22 final compounds which were evaluated in fluorometric enzyme assays for CatS inhibition and for selectivity towards the off‐targets CatB and CatL. The most potent inhibitor in the series has subnanomolar affinity (Ki=0.08 nM) and more than 100,000‐fold selectivity towards cathepsins B and L. These new reversible and non‐cytotoxic inhibitors could serve as interesting leads to develop new immunomodulators in cancer therapy.

Publisher

Wiley

Subject

Organic Chemistry,General Pharmacology, Toxicology and Pharmaceutics,Molecular Medicine,Drug Discovery,Biochemistry,Pharmacology

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