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  4. The mechanism of tumour cell death by metal-based anticancer drugs is not only a matter of DNA interactions
 
research article

The mechanism of tumour cell death by metal-based anticancer drugs is not only a matter of DNA interactions

Bergamo, Alberta
•
Dyson, Paul J.
•
Sava, Gianni
2018
Coordination Chemistry Reviews

Platinum drugs are extensively used in the clinic to treat cancer, often leading to a palliative response rather than a cure. While DNA is considered to be the primary target of platinum drugs, there is no clear relationship between cellular platinum accumulation, DNA platination and Pt-DNA adduct removal, and herein we describe new mechanistic insights of platinum drugs related to the hallmarks of cancer and how they interfere with the tumour microenvironment. We then proceed to describe the properties of other metal drugs, including both non-targeted compounds that do not significantly interact with DNA and targeted compounds that interfere more selectively with specific pathways responsible for tumour growth and invasion. Our analysis of the cancer biology and the selected drugs allows us to propose possible routes for future drug development based on metal scaffolds. (C) 2018 Elsevier B.V. All rights reserved.

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Type
research article
DOI
10.1016/j.ccr.2018.01.009
Web of Science ID

WOS:000425556700002

Author(s)
Bergamo, Alberta
Dyson, Paul J.
Sava, Gianni
Date Issued

2018

Published in
Coordination Chemistry Reviews
Volume

360

Start page

17

End page

33

Subjects

platinum drugs

•

metal-based compounds

•

cancer chemotherapy

•

dna adducts

•

molecular tumour targets

•

negative breast-cancer

•

epithelial-mesenchymal transition

•

platinum antitumor drugs

•

rna expression levels

•

regulatory t-cells

•

stem-like cells

•

lung-cancer

•

growth-factor

•

ruthenium complexes

•

nami-a

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
LCOM  
Available on Infoscience
July 11, 2018
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/147214
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