A Scaffold-Diversity Synthesis of Biologically Intriguing Cyclic Sulfonamides

Stefan Zimmermann; Mohammad Akbarzadeh; Felix Otte; Carsten Strohmann; Muthukumar Gomathi Sankar; Slava Ziegler; Axel Pahl; Sonja Sievers; Kamal Kumar

doi:10.1002/chem.201904175

A Scaffold-Diversity Synthesis of Biologically Intriguing Cyclic Sulfonamides

Chemistry. 2019 Dec 5;25(68):15498-15503. doi: 10.1002/chem.201904175. Epub 2019 Nov 7.

Authors

Stefan Zimmermann^{1

2}, Mohammad Akbarzadeh¹, Felix Otte², Carsten Strohmann², Muthukumar Gomathi Sankar¹, Slava Ziegler¹, Axel Pahl¹, Sonja Sievers¹, Kamal Kumar¹

Affiliations

¹ Abteilung Chemische Biologie, Max-Planck-Institut für Molekulare Physiologie, Otto-Hahn-Straße 11, 44227, Dortmund, Germany.
² Fakultät Chemie und Chemische Biologie, Technische Universität Dortmund, Otto-Hahn Str. 6, 44227, Dortmund, Germany.

Abstract

A "branching-folding" synthetic strategy that affords a range of diverse cyclic benzo-sulfonamide scaffolds is presented. Whereas different annulation reactions on common ketimine substrates build the branching phase of the scaffold synthesis, a common hydrogenative ring-expansion method, facilitated by an increase of the ring-strain during the branching phase, led to sulfonamides bearing medium-sized rings in a folding pathway. Cell painting assay was successfully employed to identify tubulin targeting sulfonamides as novel mitotic inhibitors.

Keywords: branching pathway; cell painting; folding pathway; mitotic inhibitors; sulfonamides.

MeSH terms

Cyclization
Sulfonamides / chemical synthesis*
Sulfonamides / chemistry

Substances

Sulfonamides

Grants and funding

115489/Innovative Medicines Initiative