Proteomics‐Based Discovery of First‐in‐Class Chemical Probes for Programmed Cell Death Protein 2 (PDCD2)

Author:

Ji Wenzhi1,Byun Woong Sub1ORCID,Lu Wenchao12,Zhu Xijun1,Donovan Katherine A.34,Dwyer Brendan G.1,Che Jianwei34,Yuan Linjie1,Abulaiti Xianmixinuer1,Corsello Steven M.1,Fischer Eric S.34,Zhang Tinghu1,Gray Nathanael S.1ORCID

Affiliation:

1. Department of Chemical and Systems Biology Chem-H and Stanford Cancer Institute Stanford School of Medicine Stanford University Stanford CA 94305 USA

2. Lingang Laboratory Shanghai 20031 China

3. Department of Cancer Biology Dana-Farber Cancer Institute Boston MA 02215 USA

4. Department of Biological Chemistry and Molecular Pharmacology Harvard Medical School Boston MA 02115 USA

Abstract

AbstractChemical probes are essential tools for understanding biological systems and for credentialing potential biomedical targets. Programmed cell death 2 (PDCD2) is a member of the B‐cell lymphoma 2 (Bcl‐2) family of proteins, which are critical regulators of apoptosis. Here we report the discovery and characterization of 10 e, a first‐in‐class small molecule degrader of PDCD2. We discovered this PDCD2 degrader by serendipity using a chemical proteomics approach, in contrast to the conventional approach for making bivalent degraders starting from a known binding ligand targeting the protein of interest. Using 10 e as a pharmacological probe, we demonstrate that PDCD2 functions as a critical regulator of cell growth by modulating the progression of the cell cycle in T lymphoblasts. Our work provides a useful pharmacological probe for investigating PDCD2 function and highlights the use of chemical proteomics to discover selective small molecule degraders of unanticipated targets.

Publisher

Wiley

Subject

General Medicine

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