Screening of Chelidonium majus isoquinoline alkaloids reveals berberine and chelidonine as selective ligands for the nuclear receptors RORβ and HNF4α, respectively

Author:

Salehi Sohrab12,Schallmayer Espen1,Bandomir Nils1,Kärcher Annette1,Güth Jan‐Frederik2,Heitel Pascal1ORCID

Affiliation:

1. Institute of Pharmaceutical Chemistry Goethe University Frankfurt Frankfurt am Main Germany

2. Department of Prosthodontics, Center for Dentistry and Oral Medicine (Carolinum) Goethe University Frankfurt Frankfurt am Main Germany

Abstract

AbstractThe nuclear receptors hepatocyte nuclear factor 4α (HNF4α) and retinoic acid receptor‐related orphan receptor‐β (RORβ) are ligand‐regulated transcription factors and potential drug targets for metabolic disorders. However, there is a lack of small molecular, selective ligands to explore the therapeutic potential in further detail. Here, we report the discovery of greater celandine (Chelidonium majus) isoquinoline alkaloids as nuclear receptor modulators: Berberine is a selective RORβ inverse agonist and modulated target genes involved in the circadian clock, photoreceptor cell development, and neuronal function. The structurally related chelidonine was identified as a ligand for the constitutively active HNF4α receptor, with nanomolar potency in a cellular reporter gene assay. In human liver cancer cells naturally expressing high levels of HNF4α, chelidonine acted as an inverse agonist and downregulated genes associated with gluconeogenesis and drug metabolism. Both berberine and chelidonine are promising tool compounds to further investigate their target nuclear receptors and for drug discovery.

Publisher

Wiley

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