Cytogenotoxic effects of two potential anticancer Ruthenium(III) Schiff Bases complexes

Cytogenotoxic effects of two potential anticancer Ruthenium(III) Schiff Bases complexes

Introduction: Treatment of cancer has been subject of great interest. Researchers are continuously searching for new medicines. In this sense, ruthenium complexes have big potential. Some evidences suggest that ruthenium compounds possess anticancer activities. We synthesized two recently published...

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Main Authors: Izet Eminovic, Emira Kahrovic, Aner Mesic, Emir Turkusic, Dzenana Kargic, Adnan Zahirovic, Zana Dolicanin
Format: Article
Language:English
Published: University of Sarajevo 2016-10-01
Series:Journal of Health Sciences
Subjects:
ruthenium
Schiff bases
anticancer agents
apoptosis
chromosome aberrations
cytogenotoxic effects
Online Access:https://www.jhsci.ba/ojs/index.php/jhsci/article/view/545
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spelling doaj-58c954896aa0440c8715d124badc1aeb2020-11-25T01:11:33ZengUniversity of SarajevoJournal of Health Sciences 2232-75761986-80492016-10-016210.17532/jhsci.2016.357197Cytogenotoxic effects of two potential anticancer Ruthenium(III) Schiff Bases complexesIzet Eminovic0Emira KahrovicAner Mesic1Emir Turkusic2Dzenana Kargic3Adnan Zahirovic4Zana Dolicanin5University of Sarajevo, Faculty of Science, Department for BiologyUniversity of Sarajevo, Faculty of Science, Department for BiologyUniversity of Sarajevo, Faculty of Science, Department for ChemistryUniversity of Sarajevo, Faculty of Science, Department for BiologyUniversity of Sarajevo, Faculty of Science, Department for ChemistryState University of Novi Pazar, Vuka Karadzica bb, 36300 Novi Pazar, Serbia Introduction: Treatment of cancer has been subject of great interest. Researchers are continuously searching for new medicines. In this sense, ruthenium complexes have big potential. Some evidences suggest that ruthenium compounds possess anticancer activities. We synthesized two recently published ruthenium(III) complexes with bidentate O,N and tridentate O,O,N Schiff bases derived from 5-substituted salicylaldehyde and aminophenol or anilineare. These compounds showed affinity for binding to the DNA molecule, however, insufficient data are available regarding their possible toxic effects on biological systems. Methods: In the present study we evaluated genotoxic, cytotoxic, and cytostatic effects of Na[RuCl2(L1)2] and Na[Ru(L2)2], using the Allium cepa assay. Results: Different toxic effects were observed depending on the substance, tested concentration, and endpoint measured. In general, the tested compounds significantly lowered the root growth and mitotic index values as compared to the control group. Additionally, a wide range of abnormal mitotic stages, both clastogenic and non-clastogenic were observed in the treated cells. Na[RuCl2(L1)2] significantly increased the frequency of sticky metaphases, chromosome bridges, micronuclei, impaired chromosome segregation, as well as number of apoptotic and necrotic cells over the controls. In contrast, Na[Ru(L2)2] did not show significant evidence of genotoxicity with regard to chromosome aberrations and micronuclei, however, significant differences were detected in the number of apoptotic and necrotic cells when the highest concentration was applied. Conclusions: In this study we demonstrated antiproliferative effects of Na[RuCl2(L1)2] and Na[Ru(L2)2]. At clinical level, these results could be interesting for further studies on anticancer potential of the ruthenium(III) complexes using animal models. https://www.jhsci.ba/ojs/index.php/jhsci/article/view/545rutheniumSchiff basesanticancer agentsapoptosischromosome aberrationscytogenotoxic effects
collection DOAJ
language English
format Article
sources DOAJ
author Izet Eminovic
Emira Kahrovic
Aner Mesic
Emir Turkusic
Dzenana Kargic
Adnan Zahirovic
Zana Dolicanin
spellingShingle Izet Eminovic
Emira Kahrovic
Aner Mesic
Emir Turkusic
Dzenana Kargic
Adnan Zahirovic
Zana Dolicanin
Cytogenotoxic effects of two potential anticancer Ruthenium(III) Schiff Bases complexes
Journal of Health Sciences
ruthenium
Schiff bases
anticancer agents
apoptosis
chromosome aberrations
cytogenotoxic effects
author_facet Izet Eminovic
Emira Kahrovic
Aner Mesic
Emir Turkusic
Dzenana Kargic
Adnan Zahirovic
Zana Dolicanin
author_sort Izet Eminovic
title Cytogenotoxic effects of two potential anticancer Ruthenium(III) Schiff Bases complexes
title_short Cytogenotoxic effects of two potential anticancer Ruthenium(III) Schiff Bases complexes
title_full Cytogenotoxic effects of two potential anticancer Ruthenium(III) Schiff Bases complexes
title_fullStr Cytogenotoxic effects of two potential anticancer Ruthenium(III) Schiff Bases complexes
title_full_unstemmed Cytogenotoxic effects of two potential anticancer Ruthenium(III) Schiff Bases complexes
title_sort cytogenotoxic effects of two potential anticancer ruthenium(iii) schiff bases complexes
publisher University of Sarajevo
series Journal of Health Sciences
issn 2232-7576
1986-8049
publishDate 2016-10-01
description Introduction: Treatment of cancer has been subject of great interest. Researchers are continuously searching for new medicines. In this sense, ruthenium complexes have big potential. Some evidences suggest that ruthenium compounds possess anticancer activities. We synthesized two recently published ruthenium(III) complexes with bidentate O,N and tridentate O,O,N Schiff bases derived from 5-substituted salicylaldehyde and aminophenol or anilineare. These compounds showed affinity for binding to the DNA molecule, however, insufficient data are available regarding their possible toxic effects on biological systems. Methods: In the present study we evaluated genotoxic, cytotoxic, and cytostatic effects of Na[RuCl2(L1)2] and Na[Ru(L2)2], using the Allium cepa assay. Results: Different toxic effects were observed depending on the substance, tested concentration, and endpoint measured. In general, the tested compounds significantly lowered the root growth and mitotic index values as compared to the control group. Additionally, a wide range of abnormal mitotic stages, both clastogenic and non-clastogenic were observed in the treated cells. Na[RuCl2(L1)2] significantly increased the frequency of sticky metaphases, chromosome bridges, micronuclei, impaired chromosome segregation, as well as number of apoptotic and necrotic cells over the controls. In contrast, Na[Ru(L2)2] did not show significant evidence of genotoxicity with regard to chromosome aberrations and micronuclei, however, significant differences were detected in the number of apoptotic and necrotic cells when the highest concentration was applied. Conclusions: In this study we demonstrated antiproliferative effects of Na[RuCl2(L1)2] and Na[Ru(L2)2]. At clinical level, these results could be interesting for further studies on anticancer potential of the ruthenium(III) complexes using animal models.
topic ruthenium
Schiff bases
anticancer agents
apoptosis
chromosome aberrations
cytogenotoxic effects
url https://www.jhsci.ba/ojs/index.php/jhsci/article/view/545
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AT emirakahrovic cytogenotoxiceffectsoftwopotentialanticancerrutheniumiiischiffbasescomplexes
AT anermesic cytogenotoxiceffectsoftwopotentialanticancerrutheniumiiischiffbasescomplexes
AT emirturkusic cytogenotoxiceffectsoftwopotentialanticancerrutheniumiiischiffbasescomplexes
AT dzenanakargic cytogenotoxiceffectsoftwopotentialanticancerrutheniumiiischiffbasescomplexes
AT adnanzahirovic cytogenotoxiceffectsoftwopotentialanticancerrutheniumiiischiffbasescomplexes
AT zanadolicanin cytogenotoxiceffectsoftwopotentialanticancerrutheniumiiischiffbasescomplexes
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