High-throughput screening and proteomic characterization of compounds targeting myeloid-derived suppressor cells

Krumm, Johannes; Petrova, Elissaveta; Lechner, Severin; Mergner, Julia; Boehm, Hans-Henning; Prestipino, Alessandro; Steinbrunn, Dominik; Deline, Marshall L.; Koetzner, Lisa; Schindler, Christina; Helming, Laura; Fromme, Tobias; Klingenspor, Martin; Hahne, Hannes; Pieck, Jan-Carsten; Kuster, Bernhard

doi:10.1016/j.mcpro.2023.100632

10.1016/j.mcpro.2023.100632

Titel:: High-throughput screening and proteomic characterization of compounds targeting myeloid-derived suppressor cells
Dokumenttyp:: Zeitschriftenaufsatz
Autor(en):: Krumm, Johannes; Petrova, Elissaveta; Lechner, Severin; Mergner, Julia; Boehm, Hans-Henning; Prestipino, Alessandro; Steinbrunn, Dominik; Deline, Marshall L.; Koetzner, Lisa; Schindler, Christina; Helming, Laura; Fromme, Tobias; Klingenspor, Martin; Hahne, Hannes; Pieck, Jan-Carsten; Kuster, Bernhard
Abstract:: Myeloid-derived suppressor cells (MDSC) are a heterogeneous cell population of incompletely differentiated immune cells. They are known to suppress T cell activity and are implicated in multiple chronic diseases, which makes them an attractive cell population for drug discovery. Here, we characterized the baseline proteomes and phospho-proteomes of mouse MDSC differentiated from a progenitor cell line to a depth of 7,000 proteins and phosphorylation sites. We also validated the cellular system for drug discovery by recapitulating and identifying known and novel molecular responses to the well-studied MDSC drugs Entinostat and Mocetinostat. We established a high-throughput drug screening platform using a MDSC/T cell co-culture system and assessed the effects of ∼21,000 small molecule compounds on T cell proliferation and INF-γ secretion to identify novel MDSC modulator. The most promising candidates were validated in a human MDSC system and subsequent proteomic experiments showed significant upregulation of several proteins associated with the reduction of reactive oxygen species (ROS). Proteome-wide solvent-induced protein stability assays identified Acyp1 und Cd74 as potential targets and the ROS reducing drug phenotype was validated by measuring ROS levels in cells in response to compound, suggesting a potential mode of action. We anticipate that the data and chemical tools developed in this study will be valuable for further research on MDSC and related drug discovery. «
Myeloid-derived suppressor cells (MDSC) are a heterogeneous cell population of incompletely differentiated immune cells. They are known to suppress T cell activity and are implicated in multiple chronic diseases, which makes them an attractive cell population for drug discovery. Here, we characterized the baseline proteomes and phospho-proteomes of mouse MDSC differentiated from a progenitor cell line to a depth of 7,000 proteins and phosphorylation sites. We also validated the cellular system f... »
Stichworte:: BayBioMS@MRI
Zeitschriftentitel:: Molecular & Cellular Proteomics
Jahr:: 2023
Seitenangaben Beitrag:: 100632
Volltext / DOI:: doi:10.1016/j.mcpro.2023.100632
Verlag / Institution:: Elsevier BV
E-ISSN:: 1535-9476
Publikationsdatum:: 01.08.2023
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