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Investigational New Drugs
Published in: Investigational New Drugs 4/2012

01-08-2012 | PRECLINICAL STUDIES

Novel acridine-based agents with topoisomerase II inhibitor activity suppress mesothelioma cell proliferation and induce apoptosis

Authors: Ahmad Raza, Blake A. Jacobson, Adam Benoit, Manish R. Patel, Joe Jay-Dixon, Hiroshi Hiasa, David M. Ferguson, Robert Arthur Kratzke

Published in: Investigational New Drugs | Issue 4/2012

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Summary

Human topoisomerase II (hTopoII) inhibitors are important chemotherapeutic agents in many different settings including treatment of malignant mesothelioma. Topoisomerase poisons, such as etoposide and doxorubicin, function by trapping the DNA-enzyme covalent complex producing DNA strand breaks which can ultimately lead to cancer cell death, as well as development of secondary malignancies. While these compounds have been used successfully in treating a wide variety of cancers, their use against mesothelioma has been limited. This study evaluates the anti-proliferative activity of series of acridine-based catalytic inhibitors of hTopoII using four mesothelioma cell lines (H513, H2372, H2461, and H2596). The results indicate these compounds inhibit malignant cell proliferation with EC50 values ranging from 6.9 to 32 μM. Experiments are also performed that show that combination therapies may be used to increase potency. Based on the results of PARP cleavage and Guava Nexin assay, it is concluded that the primary mode of cell death is by apoptosis. The results are consistent with prior work involving pancreatic cancer and hTopoII catalytic inhibitors and suggest substituted acridines may hold promise in treating malignant mesothelioma.
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Metadata
Title
Novel acridine-based agents with topoisomerase II inhibitor activity suppress mesothelioma cell proliferation and induce apoptosis
Authors
Ahmad Raza
Blake A. Jacobson
Adam Benoit
Manish R. Patel
Joe Jay-Dixon
Hiroshi Hiasa
David M. Ferguson
Robert Arthur Kratzke
Publication date
01-08-2012
Publisher
Springer US
Published in
Investigational New Drugs / Issue 4/2012
Print ISSN: 0167-6997
Electronic ISSN: 1573-0646
DOI
https://doi.org/10.1007/s10637-011-9720-7

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