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. 2024 Oct 24;67(20):18549-18575.
doi: 10.1021/acs.jmedchem.4c01926. Epub 2024 Oct 15.

First-in-Class Small Molecule Degrader of Pregnane X Receptor Enhances Chemotherapy Efficacy

Andrew D Huber  1 Young-Hwan Jung  1 Yongtao Li  1 Wenwei Lin  1 Jing Wu  1 Shyaron Poudel  1 Annalise G Carrigan  1 Ashutosh Mishra  2 Anthony A High  2 Taosheng Chen  1
Affiliations

First-in-Class Small Molecule Degrader of Pregnane X Receptor Enhances Chemotherapy Efficacy

Andrew D Huber et al. J Med Chem. .

Erratum in

Abstract

Pregnane X receptor (PXR) is a ligand-activated transcription factor that binds diverse compounds and upregulates drug metabolism machinery in response. PXR activation is detrimental to drug efficacy and safety because it reduces active drug concentrations and increases reactive metabolites, leading to toxicity and/or drug-drug interactions. Thus, effort must be expended in drug development pipelines to assess PXR activation by lead candidates and chemically modify agonists to reduce PXR liabilities while maintaining on-target potencies. Coadministration of drugs with PXR antagonists could prevent PXR-mediated metabolism events, but such compounds are rare and may themselves be converted to agonists by metabolic enzymes or PXR mutations. Here, we report the design, synthesis, optimization, and biological validation of proteolysis targeting chimeras that induce PXR degradation through E3 ubiquitin ligase recruitment. PXR degradation blocks agonist-induced gene expression and enhances anticancer effects of the chemotherapy paclitaxel, a known PXR agonist and substrate of downstream metabolic enzymes.

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Conflict of interest statement

DECLARATION OF INTERESTS

Authors T.C., A.D.H., Y.-H.J., Y.L., and W.L. declared the following competing financial interest(s): The authors have the following pending patent related to this manuscript: Small molecule degraders and fluorescent probes of PXR. The remaining authors declare no competing interests.

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