Discovery of a Potent and Highly Isoform-Selective Inhibitor of the Neglected Ribosomal Protein S6 Kinase Beta 2 (S6K2)

Author:

Gerstenecker Stefan,Haarer Lisa,Schröder MartinORCID,Kudolo Mark,Schwalm Martin P.ORCID,Wydra Valentin,Serafim Ricardo A. M.,Chaikuad ApiratORCID,Knapp StefanORCID,Laufer StefanORCID,Gehringer MatthiasORCID

Abstract

The ribosomal protein S6 kinase beta 2 (S6K2) is thought to play an important role in malignant cell proliferation, but is understudied compared to its closely related homolog S6 kinase beta 1 (S6K1). To better understand the biological function of S6K2, chemical probes are needed, but the high similarity between S6K2 and S6K1 makes it challenging to selectively address S6K2 with small molecules. We were able to design the first potent and highly isoform-specific S6K2 inhibitor from a known S6K1-selective inhibitor, which was merged with a covalent inhibitor engaging a cysteine located in the hinge region in the fibroblast growth factor receptor kinase (FGFR) 4 via a nucleophilic aromatic substitution (SNAr) reaction. The title compound shows a high selectivity over kinases with an equivalently positioned cysteine, as well as in a larger kinase panel. A good stability towards glutathione and Nα-acetyl lysine indicates a non-promiscuous reactivity pattern. Thus, the title compound represents an important step towards a high-quality chemical probe to study S6K2-specific signaling.

Funder

Baden-Württemberg Stiftung

Deutsche Forschungsgemeinschaft

Verband der Chemischen Industrie

Max-Buchner-Forschungsstiftung

Ministerium für Wissenschaft, Forschung und Kunst Baden-Württemberg

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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