Development of Light‐Activated LXR Agonists

Author:

Mukhopadhyay Tufan K.1ORCID,Willems Sabine2ORCID,Arp Christopher J.1ORCID,Morstein Johannes1,Haake Caleb T.1,Merk Daniel2ORCID,Trauner Dirk3ORCID

Affiliation:

1. Department of Chemistry New York University New York City, NY 10003 USA

2. Department of Pharmacy Ludwig-Maximilians-Universität München Butenandtstraße 5–13 81377 Munich Germany

3. Department of Chemistry University of Pennsylvania College of Arts and Sciences 231 South 34th Street Philadelphia PA 19104-6323 USA

Abstract

AbstractActivation of the oxysterol‐sensing transcription factor liver X receptor (LXR) has been studied as a therapeutic strategy in metabolic diseases and cancer but is compromised by the side effects of LXR agonists. Local LXR activation in cancer treatment may offer an opportunity to overcome this issue suggesting potential uses of photopharmacology. We report the computer‐aided development of photoswitchable LXR agonists based on the T0901317 scaffold, which is a known LXR agonist. Azologization and structure‐guided structure‐activity relationship evaluation enabled the design of an LXR agonist, which activated LXR with low micromolar potency in its light‐induced (Z)‐state and was inactive as (E)‐isomer. This tool sensitized human lung cancer cells to chemotherapeutic treatment in a light‐dependent manner supporting potential of locally activated LXR agonists as adjuvant cancer treatment.

Funder

National Institutes of Health

Publisher

Wiley

Subject

Organic Chemistry,General Pharmacology, Toxicology and Pharmaceutics,Molecular Medicine,Drug Discovery,Biochemistry,Pharmacology

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