Activity-Based Protein Profiling of RHBDL4 Reveals Proteolysis of the Enzyme and a Distinct Inhibitor Profile

Authors

Cassondra C. Davies, Oberlin College
Ren-Ming Hu
Paul J. Kamitsuka, Oberlin College
Gabriel N. Morais, Oberlin College
Regina Stasser de Gonzalez, Oberlin College
Katelyn A. Bustin, Oberlin College
Megan L. Matthews
William Parsons, Oberlin College

Abstract

Rhomboid proteases have fascinated scientists by virtue of their membrane-embedded active sites and proposed involvement in physiological and disease pathways. The human rhomboid protease RHBDL4 has generated particular interest due to its role in endoplasmic reticulum-associated protein degradation and upregulation in several cancers; however, chemical tools for studying this enzyme are currently lacking. Here, we describe the development of an activity-based protein profiling (ABPP) assay for RHBDL4. We have employed this assay to determine that human RHBDL4 undergoes proteolytic processing in cells to produce multiple active proteoforms with truncated C-termini. We have also used this assay to identify chemical scaffolds capable of inhibiting RHBDL4 activity and have observed distinct inhibitor preferences between RHBDL4 and a second human rhomboid protease PARL. Our work demonstrates the power of ABPP technology to characterize active forms of enzymes that might otherwise elude detection and the potential to achieve selective inhibition among the human rhomboid proteases.

Repository Citation

Davies, Cassondra C., Ren-Ming Hu, Paul J. Kamitsuka, et al. 2024. "Activity-Based Protein Profiling of RHBDL4 Reveals Proteolysis of the Enzyme and a Distinct Inhibitor Profile." ACS Chemical Biology 19(8): 1674-1682.

Publisher

American Chemical Society

Publication Date

7-23-2024

Publication Title

ACS Chemical Biology

Department

Chemistry and Biochemistry

Document Type

Article

DOI

https://dx.doi.org/10.1021/acschembio.4c00273

Keywords

Rhomboid proteases, Family

Language

English

Format

text