Synthesis and Evaluation of N-Arylsulfonylated Succinimides as Activity-Based Probes

Authors

Jo Chvatal, Oberlin College
Dat T. Nguyen, Oberlin College
Alexondra S. Xie, Oberlin College
William H. Parsons, Oberlin College

Abstract

Activity-based protein profiling (ABPP) technology has served as a powerful platform for studying proteins for more than two decades. However, the further growth of this field depends on the development of new probe structures to expand the proportion of the proteome that can be studied using these methods. Inspired by previous reports of succinimide-containing covalent inhibitors for proteases, we synthesized a panel of potential probe structures with a succinimide reactive group and a terminal alkyne tag suitable for subsequent azide-alkyne click chemistry. Members of this panel with an N-arylsulfonyl linker produce labeling of both purified serine proteases as well as proteins in complex cellular lysates. We found that one of these probes labels the human rhomboid protease RHBDL2 at low micromolar concentrations and can be competed with active-site inhibitors. Our studies establish succinimide as a new reactive group for the development of activity-based probes and offer a new chemical tool for studying a class of enzymes with limited functional characterization.

Repository Citation

Chvatal, Jo, Dat T. Nguyen, Alexondra S. Xie, and William H. Parsons. 2025. "Synthesis and Evaluation of N-Arylsulfonylated Succinimides as Activity-Based Probes." Synlett 36(16): 2603-2608.

Publisher

Georg Thieme Verlag KG

Publication Date

10-1-2025

Publication Title

Synlett

Department

Chemistry and Biochemistry

Document Type

Article

DOI

https://doi.org/10.1055/s-0043-1775487

Keywords

Chemical probes, Click chemistry, Succinimides

Language

English

Format

text