Exploiting bioactive natural products of marine origin: Evaluation of the meroterpenoid metachromin V as a novel potential therapeutic drug for colorectal cancer

Donatella Lucchetti, Francesca Luongo, Filomena Colella, Enrico Gurreri, Giulia Artemi, Claudia Desiderio, Stefano Serra, Felice Giuliante, Ruggero De Maria Marchiano, Alessandro Sgambato*, Alberto Vitali, Micol Eleonora Fiori

*Autore corrispondente per questo lavoro

Risultato della ricerca: Contributo in rivistaArticolo

Abstract

Colorectal cancer (CRC) is the second most common cause of cancer death, leading to almost 1 million deaths per year. Despite constant progress in surgical and therapeutic protocols, the 5-year survival rate of advanced CRC patients remains extremely poor. Colorectal Cancer Stem Cells (CRC-CSCs) are endowed with unique stemness-related properties responsible for resistance, relapse and metastasis. The development of novel therapeutics able to tackle CSCs while avoiding undesired toxicity is a major need for cancer treatment. Natural products are a large reservoir of unexplored compounds with possible anticancer bioactivity, sustainability, and safety. The family of meroterpenoids derived from sponges share interesting bioactive properties. Bioassay-guided frac-tionation of a meroterpenoids extract led to the isolation of three compounds, all cytotoxic against several cancer cell lines: Metachromins U, V and W. In this study, we evaluated the anticancer potential of the most active one, Metachromins V (MV), on patient-derived CRC-CSCs. MV strongly impairs CSCs-viability regardless their mutational background and the cytotoxic effect is maintained on therapy-resistant metastatic CSCs. MV affects cell cycle progression, inducing a block in G2 phase in all the cell lines tested and more pronouncedly in CRC-CSCs. Moreover, MV triggers an important reorganization of the cytoskeleton and a strong reduction of Rho GTPases expression, impairing CRC-CSCs motility and invasion ability. By Proteomic analysis identified a po-tential molecular target of MV: CCAR1, that regulates apoptosis under chemotherapy treatments and affect beta-catenin pathway. Further studies will be needed to confirm and validate these data in in vivo experimental models
Lingua originaleInglese
pagine (da-a)114679-114690
Numero di pagine12
RivistaBIOMEDICINE & PHARMACOTHERAPY
Volume162
DOI
Stato di pubblicazionePubblicato - 2023

Keywords

  • Cancer stem cells
  • Colorectal cancer
  • Natural products
  • Therapeutic drug

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