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  3. In vitro and in vivo activities of a trithiolato-diRuthenium complex conjugated with sulfadoxine against the apicomplexan parasite Toxoplasma gondii.
 

In vitro and in vivo activities of a trithiolato-diRuthenium complex conjugated with sulfadoxine against the apicomplexan parasite Toxoplasma gondii.

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BORIS DOI
10.48350/196531
Publisher DOI
10.1016/j.ijpddr.2024.100544
PubMed ID
38703737
Description
Organometallic compounds, including Ruthenium complexes, have been widely developed as anti-cancer chemotherapeutics, but have also attracted much interest as potential anti-parasitic drugs. Recently hybrid drugs composed of organometallic Ruthenium moieties that were complexed to different antimicrobial agents were synthesized. One of these compounds, a trithiolato-diRuthenium complex (RU) conjugated to sulfadoxine (SDX), inhibited proliferation of Toxoplasma gondii tachyzoites grown in human foreskin fibroblast (HFF) monolayers with an IC50 < 150 nM, while SDX and the non-modified RU complex applied either individually or as an equimolar mixture were much less potent. In addition, conjugation of SDX to RU lead to decreased HFF cytotoxicity. RU-SDX did not impair the in vitro proliferation of murine splenocytes at concentrations ranging from 0.1 to 0.5 μM but had an impact at 2 μM, and induced zebrafish embryotoxicity at 20 μM, but not at 2 or 0.2 μM. RU-SDX acted parasitostatic but not parasiticidal, and induced transient ultrastructural changes in the mitochondrial matrix of tachyzoites early during treatment. While other compounds that target the mitochondrion such as the uncouplers FCCP and CCCP and another trithiolato-Ruthenium complex conjugated to adenine affected the mitochondrial membrane potential, no such effect was detected for RU-SDX. Evaluation of the in vivo efficacy of RU-SDX in a murine T. gondii oocyst infection model comprised of non-pregnant outbred CD1 mice showed no effects on the cerebral parasite burden, but reduced parasite load in the eyes and in heart tissue.
Date of Publication
2024-08
Publication Type
Article
Subject(s)
600 Technology > 630 Agriculture
500 Science > 570 Life sciences; biology
500 Science > 540 Chemistry
000 Computer science, knowledge & systems
Keyword(s)
Cytotoxicity In vivo efficacy Organometallic drugs Proliferation inhibition Splenocytes Sulfadoxine Toxoplasma Transmission electron microscopy Trithiolato diruthenium complex
Language(s)
en
Contributor(s)
Boubaker, Ghalia
Institut für Parasitologie (IPA) - Gruppe Hemphill
Institut für Parasitologie (IPA)
Bernal, Alice Jeanine Felisa
Institut für Parasitologie (IPA)
Vigneswaran, Anitha
Institut für Parasitologie (IPA)
Imhof, Dennisorcid-logo
Institut für Parasitologie (IPA)
Institut für Parasitologie (IPA) - Gruppe Hemphill
Ferreira de Sousa, Maria Cristina
Institut für Parasitologie (IPA) - Gruppe Hemphill
Institut für Parasitologie (IPA)
Hänggeli, Kai Pascal Alexanderorcid-logo
Institut für Parasitologie (IPA)
Institut für Parasitologie (IPA) - Gruppe Hemphill
Haudenschild, Noé Marc
Institut für Parasitologie (IPA)
Furrer, Julienorcid-logo
DCBP Gruppe Prof. Furrer
Departement für Chemie, Biochemie und Pharmazie (DCBP) Universität Bern
Paunescu, Emilia
Departement für Chemie, Biochemie und Pharmazie (DCBP) Universität Bern
Desiatkina, Oksana
Departement für Chemie, Biochemie und Pharmazie (DCBP) Universität Bern
Hemphill, Andrew
Institut für Parasitologie (IPA)
Institut für Parasitologie (IPA) - Gruppe Hemphill
Additional Credits
Microscopy Imaging Center (MIC)
Institut für Parasitologie (IPA)
Institut für Parasitologie (IPA) - Gruppe Hemphill
Departement für Chemie, Biochemie und Pharmazie (DCBP) Universität Bern
DCBP Gruppe Prof. Furrer
Series
International journal for parasitology. Drugs and drug resistance
Publisher
Elsevier
ISSN
2211-3207
Access(Rights)
open.access
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