Novel ruthenium(II) cyclopentadienyl thiosemicarbazone compounds with antiproliferative activity on pathogenic trypanosomatid parasites

被引:37
|
作者
Fernandez, Mariana [1 ]
Arce, Esteban Rodriguez [1 ]
Sarniguet, Cynthia [1 ]
Morais, Tania S. [2 ]
Tomaz, Ana Isabel [2 ]
Azar, Claudio Olea [3 ]
Figueroa, Roberto [3 ]
Diego Maya, J. [4 ]
Medeiros, Andrea [5 ,6 ]
Comini, Marcelo [5 ]
Garcia, M. Helena [2 ]
Otero, Lucia [1 ]
Gambino, Dinorah [1 ]
机构
[1] Univ Republica, Fac Quim, Catedra Quim Inorgan, Montevideo, Uruguay
[2] Univ Lisbon, Fac Ciencias, Ctr Quim Estrutural, Lisbon, Portugal
[3] Univ Chile, Fac Ciencias Quim & Farmaceut, Dept Quim Inorgan & Analit, Santiago, Chile
[4] Univ Chile, Fac Med, Programa Farmacol Mol & Clin, ICBM, Santiago 7, Chile
[5] Grp Redox Biol Trypanosomes, Inst Pasteur Montevideo, Montevideo, Uruguay
[6] Univ Republica, Fac Med, Dept Bioquim, Montevideo, Uruguay
关键词
Ruthenium cyclopentadienyl compounds; Thiosemicarbazones; Trypanosoma cruzi; Trypanosoma brucei; IN-VITRO ANTIMALARIAL; TROPICAL DISEASES; CHAGAS-DISEASE; ANTITRYPANOSOMAL ACTIVITY; HETEROAROMATIC LIGANDS; DERIVATIVE COMPLEXES; METAL-COMPLEXES; NUCLEIC-ACIDS; BLOOD-STREAM; DNA-BINDING;
D O I
10.1016/j.jinorgbio.2015.06.018
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Searching for new prospective antitrypanosomal agents, three novel Ru(II)-cyclopentadienyl compounds, [Ru(eta(5)-C5H5)(PPh3)L], with HL = bioactive 5-nitrofuryl containing thiosemicarbazones were synthesized and characterized in the solid state and in solution. The compounds were evaluated in vitro on the blood circulating trypomastigote form of Trypanosoma cruzi (Dm28c strain), the infective form of Trypanosoma brucei brucei (strain 427) and on J774 murine macrophages and human-derived EA.hy926 endothelial cells. The compounds were active against both parasites with IC50 values in the micromolar or submicromolar range. Interestingly, they are much more active on T. cruzi than previously developed Ru(II) classical and organometallic compounds with the same bioactive ligands. The new compounds showed moderate to very good selectivity towards the parasites in respect to mammalian cells. The global results point at [RuCp(PPh3)L2] (12 = N-methyl derivative of 5-nitrofuryl containing thiosemicarbazone and Cp = cyclopentadienyl) as the most promising compound for further developments (IC50 T. cruzi = 0.41 mu M; IC50 T. brucei brucei = 3.5 mu M). Moreover, this compound shows excellent selectivity towards T. cruzi (SI > 49) and good selectivity towards T. brucei brucei (SI > 6). In order to get insight into the mechanism of antiparasitic action, the intracellular free radical production capacity of the new compounds was assessed by ESR. DMPO (5,5-dimethyl-1-pirroline-N-oxide) spin adducts related to the bioreduction of the complexes and to redox cycling processes were characterized. In addition, DNA competitive binding studies with ethidium bromide by fluorescence measurements showed that the compounds interact with this biomolecule. (C) 2015 Elsevier Inc. All rights reserved.
引用
收藏
页码:306 / 314
页数:9
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