Publication:
Discovery of a Novel, Isothiazolonaphthoquinone-Based Small Molecule Activator of FOXO Nuclear-Cytoplasmic Shuttling

No Thumbnail Available

Date

2016-12-09

Authors

Cautain, Bastien
Castillo, Francisco
Musso, Loana
Ferreira, Bibiana I.
de Pedro, Nuria
Quesada, Lorena Rodriguez
Machado, Susana
Vicente, Francisca
Dallavalle, Sabrina
Link, Wolfgang

Advisors

Journal Title

Journal ISSN

Volume Title

Publisher

Public library science
Metrics
Google Scholar
Export

Research Projects

Organizational Units

Journal Issue

Abstract

FOXO factors are tumour suppressor proteins commonly inactivated in human tumours by posttranslational modifications. Furthermore, genetic variation within the FOXO3a gene is consistently associated with human longevity. Therefore, the pharmacological activation of FOXO proteins is considered as an attractive therapeutic approach to treat cancer and age-related diseases. In order to identify agents capable of activating FOXOs, we tested a collection of small chemical compounds using image-based high content screening technology. Here, we report the discovery of LOM612 (compound 1a), a newly synthesized isothiazolonaphthoquinone as a potent FOXO relocator. Compound 1a induces nuclear translocation of a FOXO3a reporter protein as well as endogenous FOXO3a and FOXO1 in U2OS cells in a dose-dependent manner. This activity does not affect the subcellular localization of other cellular proteins including NFkB or inhibit CRM1-mediated nuclear export. Furthermore, compound 1a shows a potent antiproliferative effect in human cancer cell lines.

Description

MeSH Terms

DeCS Terms

CIE Terms

Keywords

Forkhead transcription factor, Dual-specificity phosphatase, Cycloaddition reactions, Nitrile sulfides, Inhibitors, Cancer, Translocation, Screen, Potent, Cells

Citation