Issue 80, 2019
From the journal:

Chemical Communications

Anticancer organorhodium and -iridium complexes with low toxicity in vivo but high potency in vitro: DNA damage, reactive oxygen species formation, and haemolytic activity

Shahida Parveen,a   Muhammad Hanif, ORCID logo *a   Euphemia Leung, ORCID logo b   Kelvin K. H. Tong, ORCID logo a   Annie Yang,c   Jonathan Astin,c   Gayan H. De Zoysa, ORCID logo a   Tasha R. Steel,a   David Goodman, ORCID logo a   Sanam Movassaghi,a   Tilo Söhnel, ORCID logo a   Vijayalekshmi Sarojini, ORCID logo a   Stephen M. F. Jamieson ORCID logo b  and  Christian G. Hartinger ORCID logo *a  

* Corresponding authors

a School of Chemical Sciences, University of Auckland, Private Bag 92019, Auckland 1142, New Zealand
E-mail: c.hartinger@auckland.ac.nz, m.hanif@auckland.ac.nz
Web: http://www.hartinger.auckland.ac.nz/

b Auckland Cancer Society Research Centre, University of Auckland, Private Bag 92019, Auckland 1142, New Zealand

c Department of Molecular Medicine and Pathology, University of Auckland, Private Bag 92019, Auckland 1142, New Zealand

Abstract

Redox-modulating anticancer drugs allow the exploitation of altered redox biology observed in many cancer cells. We discovered dinuclear RhIII(Cp*) and IrIII(Cp*) complexes that have in vitro anticancer activity superior to cisplatin and the investigational drug IT-139, while being less toxic in haemolysis and in vivo zebrafish models. The mode of action appears to be related to DNA damage and ROS-mediated stress pathways.

Graphical abstract: Anticancer organorhodium and -iridium complexes with low toxicity in vivo but high potency in vitro: DNA damage, reactive oxygen species formation, and haemolytic activity

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Article information

DOI
https://doi.org/10.1039/C9CC03822A
Article type
Communication
Submitted
17 mai 2019
Accepted
29 août 2019
First published
30 août 2019

Chem. Commun., 2019,55, 12016-12019

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Anticancer organorhodium and -iridium complexes with low toxicity in vivo but high potency in vitro: DNA damage, reactive oxygen species formation, and haemolytic activity

S. Parveen, M. Hanif, E. Leung, K. K. H. Tong, A. Yang, J. Astin, G. H. De Zoysa, T. R. Steel, D. Goodman, S. Movassaghi, T. Söhnel, V. Sarojini, S. M. F. Jamieson and C. G. Hartinger, Chem. Commun., 2019, 55, 12016 DOI: 10.1039/C9CC03822A

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