Synthesis and biological evaluation of novel FiVe1 derivatives as potent and selective agents for the treatment of mesenchymal cancers

Francisco Martínez-Peña; Aaron D Pearson; Eileen L Tang; Nick A Kuburich; Sendurai A Mani; Peter G Schultz; Michael J Bollong; Luke L Lairson

doi:10.1016/j.ejmech.2022.114638

Synthesis and biological evaluation of novel FiVe1 derivatives as potent and selective agents for the treatment of mesenchymal cancers

Eur J Med Chem. 2022 Nov 15:242:114638. doi: 10.1016/j.ejmech.2022.114638. Epub 2022 Aug 6.

Authors

Francisco Martínez-Peña¹, Aaron D Pearson¹, Eileen L Tang¹, Nick A Kuburich², Sendurai A Mani², Peter G Schultz¹, Michael J Bollong³, Luke L Lairson⁴

Affiliations

¹ Department of Chemistry, The Scripps Research Institute, La Jolla, CA, 92037, USA.
² Department of Translational Molecular Pathology, The University of Texas, MD, Anderson, USA.
³ Department of Chemistry, The Scripps Research Institute, La Jolla, CA, 92037, USA. Electronic address: mbollong@scripps.edu.
⁴ Department of Chemistry, The Scripps Research Institute, La Jolla, CA, 92037, USA. Electronic address: llairson@scripps.edu.

Abstract

Epithelial-mesenchymal transition (EMT) endows stem cell-like properties to cancer cells. Targeting this process represents a potential therapeutic approach to overcome cancer metastasis and chemotherapy resistance. FiVe1 was identified from an EMT-based synthetic lethality screen and was found to inhibit the stem cell-like properties and proliferation of not only cancer cells undergoing EMT, but also more broadly in mesenchymal cancers that include therapeutically intractable soft tissue sarcomas. FiVe1 functions by directly binding to the type III intermediate filament protein vimentin (VIM) in a mode that induces hyperphosphorylation of Ser56, which results in selective disruption of mitosis and induced multinucleation in transformed VIM-expressing mesenchymal cancer cell types. Cell-based potency (IC₅₀ = 1.6 μM, HT-1080 fibrosarcoma), poor solubility (<1 μM) and low oral bioavailability limits the direct application of FiVe1 as an in vivo probe or therapeutic agent. To overcome these drawbacks, we performed structure-activity relationship (SAR) studies and synthesized a set of 35 new compounds, consisting of diverse modifications of the FiVe1 scaffold. Among these compounds, 4e showed a marked improvement in potency (IC₅₀ = 44 nM, 35-fold improvement, HT-1080) and cell type selectivity (19-fold improvement), when compared to FiVe1. Improvements in the potency of 4e, in terms of overall cytotoxicity, directly correlate with VIM Ser56 phosphorylation status and the oral bioavailability and pharmacokinetic profiles of 4e in mouse are superior to FiVe1. Successful optimization also resulted in potent and selective derivatives 11a, 11j and 11k, which exhibited superior pharmacological profiles, in terms of metabolic stability and aqueous solubility. Collectively, these optimization efforts have resulted in the development of promising FiVe1 analogs with potential applications in the treatment of mesenchymal cancers, as well as in the study of VIM-related biology.

Keywords: Medicinal chemistry; Mesenchymal cancer; Structure-activity relationship; Vimentin.

MeSH terms

Animals
Cell Line, Tumor
Epithelial-Mesenchymal Transition*
Mice
Mitosis
Phosphorylation
Sarcoma*
Vimentin / genetics

Substances

Vimentin

Grants and funding

R01 CA200970/CA/NCI NIH HHS/United States