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Thiosemicarbazones Can Act Synergistically with Anthracyclines to Downregulate CHEK1 Expression and Induce DNA Damage in Cell Lines Derived from Pediatric Solid Tumors
S. Paukovcekova, M. Krchniakova, P. Chlapek, J. Neradil, J. Skoda, R. Veselska
Language English Country Switzerland
Document type Journal Article
Grant support
17-33104A
Ministry of Health
MUNI/A/1522/2020
Masaryk University
MUNI/A/1325/2021
Masaryk University
CZ.02.1.01/0.0/0.0/16_019/0000868
European Regional Development Fund
LX22NPO5102
European Union - Next Generation EU
NLK
Free Medical Journals
from 2000
Freely Accessible Science Journals
from 2000
PubMed Central
from 2007
Europe PubMed Central
from 2007
ProQuest Central
from 2000-03-01
Open Access Digital Library
from 2000-01-01
Open Access Digital Library
from 2007-01-01
Health & Medicine (ProQuest)
from 2000-03-01
ROAD: Directory of Open Access Scholarly Resources
from 2000
PubMed
35955683
DOI
10.3390/ijms23158549
Knihovny.cz E-resources
- MeSH
- Anthracyclines * pharmacology MeSH
- Checkpoint Kinase 1 metabolism MeSH
- Child MeSH
- Doxorubicin metabolism pharmacology MeSH
- Topoisomerase II Inhibitors MeSH
- Humans MeSH
- Cell Line, Tumor MeSH
- ATP Binding Cassette Transporter, Subfamily B, Member 1 metabolism MeSH
- DNA Damage MeSH
- Antibiotics, Antineoplastic MeSH
- Thiosemicarbazones * pharmacology MeSH
- Check Tag
- Child MeSH
- Humans MeSH
- Publication type
- Journal Article MeSH
Anticancer therapy by anthracyclines often leads to the development of multidrug resistance (MDR), with subsequent treatment failure. Thiosemicarbazones have been previously suggested as suitable anthracycline partners due to their ability to overcome drug resistance through dual Pgp-dependent cytotoxicity-inducing effects. Here, we focused on combining anthracyclines (doxorubicin, daunorubicin, and mitoxantrone) and two thiosemicarbazones (DpC and Dp44mT) for treating cell types derived from the most frequent pediatric solid tumors. Our results showed synergistic effects for all combinations of treatments in all tested cell types. Nevertheless, further experiments revealed that this synergism was independent of Pgp expression but rather resulted from impaired DNA repair control leading to cell death via mitotic catastrophe. The downregulation of checkpoint kinase 1 (CHEK1) expression by thiosemicarbazones and the ability of both types of agents to induce double-strand breaks in DNA may explain the Pgp-independent synergism between anthracyclines and thiosemicarbazones. Moreover, the concomitant application of these agents was found to be the most efficient approach, achieving the strongest synergistic effect with lower concentrations of these drugs. Overall, our study identified a new mechanism that offers an avenue for combining thiosemicarbazones with anthracyclines to treat tumors regardless the Pgp status.
Department of Experimental Biology Faculty of Science Masaryk University 61137 Brno Czech Republic
International Clinical Research Center St Anne's University Hospital 65691 Brno Czech Republic
References provided by Crossref.org
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