Communications Biology (Mar 2024)

Platinum iodido drugs show potential anti-tumor activity, affecting cancer cell metabolism and inducing ROS and senescence in gastrointestinal cancer cells

  • Jorge Melones-Herrero,
  • Sonia Alcalá,
  • Laura Ruiz-Cañas,
  • Carlos Benítez-Buelga,
  • Sandra Batres-Ramos,
  • Carmela Calés,
  • Oscar Lorenzo,
  • Rosario Perona,
  • Adoración G. Quiroga,
  • Bruno Sainz,
  • Isabel Sánchez-Pérez

DOI
https://doi.org/10.1038/s42003-024-06052-5
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 16

Abstract

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Abstract Cisplatin-based chemotherapy has associated clinical disadvantages, such as high toxicity and resistance. Thus, the development of new antitumor metallodrugs able to overcome different clinical barriers is a public healthcare priority. Here, we studied the mechanism of action of the isomers trans and cis-[PtI2(isopropylamine)2] (I5 and I6, respectively) against gastrointestinal cancer cells. We demonstrate that I5 and I6 modulate mitochondrial metabolism, decreasing OXPHOS activity and negatively affecting ATP-linked oxygen consumption rate. Consequently, I5 and I6 generated Reactive Oxygen Species (ROS), provoking oxidative damage and eventually the induction of senescence. Thus, herein we propose a loop with three interconnected processes modulated by these iodido agents: (i) mitochondrial dysfunction and metabolic disruptions; (ii) ROS generation and oxidative damage; and (iii) cellular senescence. Functionally, I5 reduces cancer cell clonogenicity and tumor growth in a pancreatic xenograft model without systemic toxicity, highlighting a potential anticancer complex that warrants additional pre-clinical studies.