Induction of the Endoplasmic Reticulum Stress Pathway by Highly Cytotoxic Organoruthenium Schiff-Base Complexes

Research output: Journal Publications and Reviews (RGC: 21, 22, 62)21_Publication in refereed journalpeer-review

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Author(s)

  • Mun Juinn Chow
  • Kwan Wei Tan
  • Mei Chi Cheong
  • Giorgia Pastorin
  • Christian Gaiddon
  • Wee Han Ang

Detail(s)

Original languageEnglish
Pages (from-to)3020-3031
Journal / PublicationMolecular Pharmaceutics
Volume15
Issue number8
Online published6 Jul 2018
Publication statusPublished - 6 Aug 2018
Externally publishedYes

Abstract

Current anticancer drug discovery efforts focus on the identification of first-in-class compounds with a mode-of-action distinct from conventional DNA-targeting agents for chemotherapy. An emerging trend is the identification of endoplasmic reticulum (ER) targeting compounds that induce ER stress in cancer cells, leading to cell death. However, a limited pool of such compounds has been identified to date, and there are limited studies done on such compounds to allow for the rational design of ER stress-inducing agents. In our present study, we present a series of highly cytotoxic, ER stress-inducing Ru(II)-arene Schiff-Base (RAS) complexes, bearing iminoquinoline chelate ligands. We demonstrate that by structural modification to the iminoquinoline ligand, we could tune its π-acidity and influence reactive oxygen species (ROS) induction, switching between a ROS-mediated ER stress pathway activation and one that is not mediated by ROS induction. Our current study adds to the available ER stress inducers and shows how structural tuning could be used as a means to modulate the mode-of-action of such compounds.

Research Area(s)

  • anticancer, endoplasmic reticulum stress, p53-independent activity, reactive oxygen species, ruthenium arene Schiff-base complexes

Citation Format(s)

Induction of the Endoplasmic Reticulum Stress Pathway by Highly Cytotoxic Organoruthenium Schiff-Base Complexes. / Chow, Mun Juinn; Babak, Maria V.; Tan, Kwan Wei et al.

In: Molecular Pharmaceutics, Vol. 15, No. 8, 06.08.2018, p. 3020-3031.

Research output: Journal Publications and Reviews (RGC: 21, 22, 62)21_Publication in refereed journalpeer-review