Synthesis, Characterization And Antitumor Activity OfCopper(II) Complexes, [CuL 2 ] [HL 1-3 =N,N‐Diethyl‐N′‐(R‐Benzoyl)Thiourea (R=H, o‐Cl and p‐NO 2 )]

The copper (II) complexes (CuL 2 ) were prepared by reaction of with the corresponding derivatives of acylthioureas in a Cu:HL molar ratio of 1:2. Acylthiourea ligands, N,N‐diethyl‐N′‐(R‐benzoyl) thiourea (HL 1-3 ) [R=H, o‐Cl and p‐NO 2 ] were synthesized in high yield (78‐83%) and characterized by...

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Veröffentlicht in:Bioinorganic chemistry and applications 2005-01, Vol.3 (3-4), p.299-316
Hauptverfasser: Hernández, Wilfredo, Spodine, Evgenia, Beyer, Lothar, Schröder, Uwe, Richter, Rainer, Ferreira, Jorge, Pavani, Mario
Format: Artikel
Sprache:eng ; jpn
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Zusammenfassung:The copper (II) complexes (CuL 2 ) were prepared by reaction of with the corresponding derivatives of acylthioureas in a Cu:HL molar ratio of 1:2. Acylthiourea ligands, N,N‐diethyl‐N′‐(R‐benzoyl) thiourea (HL 1-3 ) [R=H, o‐Cl and p‐NO 2 ] were synthesized in high yield (78‐83%) and characterized by elemental analysis, infrared spectroscopy, 1 H and 13 C NMR spectroscopy. The complexes CuL 2 were characterized by elemental analysis, IR, FAB(+)‐MS, magnetic susceptibility measurements, EPR and cyclic voltammetry. The crystal structure of the complex Cu(L 2 ) 2 shows a nearly square‐planar geometry with two deprotonated ligands (L) coordinated to Cu II through the oxygen and sulfur atoms in a cis arrangement. The antitumor activity of the copper(II) complexes with acylthiourea ligands was evaluated in vitro against the mouse mammary adenocarcinoma TA3 cell line. These complexes exhibited much higher cytotoxic activity (IC 50 values in the range of 3.9‐6.9 μM) than their corresponding ligands (40‐240 μM), which indicates that the coordination of the chelate ligands around the Cu II enhances the antitumor activity and, furthermore, this result confirmed that the participation of the nitro and chloro substituent groups in the complex activities is slightly relevant. The high accumulation of the complexes Cu(L 2 ) 2 and Cu(L 3 ) 2 in TA3 tumor cells and the much faster binding to cellular DNA than Cu(L 1 ) 2 are consistent with the in vitro cytotoxic activities found for these copper complexes.
ISSN:1565-3633
1687-479X
DOI:10.1155/BCA.2005.299