Selection of Natural Compounds with HMGA-Interfering Activities and Cancer Cell Cytotoxicity

Overview

Journal ACS Omega

Publisher American Chemical Society

Specialty Chemistry

Date 2023 Sep 18

PMID 37720761

Authors

Mattia Mori

Francesca Ghirga

Beatrice Amato

Luca Secco

Deborah Quaglio

Isabella Romeo

Marta Gambirasi

Alberta Bergamo

Sonia Covaceuszach

Riccardo Sgarra

Bruno Botta

Guidalberto Manfioletti

Affiliations

Soon will be listed here.

Abstract

HMGA proteins are intrinsically disordered (ID) chromatin architectural factors characterized by three DNA binding domains (AT-hooks) that allow them to bind into the DNA minor groove of AT-rich stretches. HMGA are functionally involved in regulating transcription, RNA processing, DNA repair, and chromatin remodeling and dynamics. These proteins are highly expressed and play essential functions during embryonic development. They are almost undetectable in adult tissues but are re-expressed at high levels in all cancers where they are involved in neoplastic transformation and cancer progression. We focused on identifying new small molecules capable of binding into the minor groove of AT-rich DNA sequences that could compete with HMGA for DNA binding and, thus, potentially interfere with their activities. Here, a docking-based virtual screening of a unique high diversity in-house library composed of around 1000 individual natural products identified 16 natural compounds as potential minor groove binders that could inhibit the interaction between HMGA and DNA. To verify the ability of these selected compounds to compete with HMGA proteins, we screened them using electrophoretic mobility shift assays. We identified Sorocein C, a Diels-Alder (D-A)-type adducts, isolated from and with an HMGA/DNA-displacing activity and compared its activity with that of two structurally related compounds, Sorocein A and Sorocein B. All these compounds showed a cytotoxicity effect on cancer cells, suggesting that the Sorocein-structural family may provide new and yet unexplored chemotypes for the development of minor groove binders to be evaluated as anticancer agents.

Citing Articles

Crystal structure of the HMGA AT-hook 1 domain bound to the minor groove of AT-rich DNA and inhibition by antikinetoplastid drugs.

Nue-Martinez J, Maturana M, Lagartera L, Rodriguez-Gutierrez J, Boer R, Campos J Sci Rep. 2024; 14(1):26173.

PMID: 39478017 PMC: 11526092. DOI: 10.1038/s41598-024-77522-3.

Binding to the Other Side: The AT-Hook DNA-Binding Domain Allows Nuclear Factors to Exploit the DNA Minor Groove.

Battista S, Fedele M, Secco L, Ingo A, Sgarra R, Manfioletti G Int J Mol Sci. 2024; 25(16).

PMID: 39201549 PMC: 11354804. DOI: 10.3390/ijms25168863.

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