Preparation, characterization, and anticancer activity of a series of cis-PtCl2 complexes linked to anthraquinone intercalators

A new series of complexes of the type cis-PtL2X2 [where L is a monodentate AQ-Y(CH2)nNH2 and L2 is a bidentate AQ-Y(CH2)nNH(CH2)2NH2; AQ = anthraquinone, X = Cl, I, Y = NH, O] in which anthraquinone intercalators are tethered to the cis-PtCl2 unit via an (aminoalkyl)amino, (oxyalkyl)amino, or polyet...

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Bibliographic Details
Published in:Journal of medicinal chemistry 1991-01, Vol.34 (1), p.414-420
Main Authors: Gibson, Dan, Gean, Keria Fiorella, Katzhendle, Jehoshua, Ben-Shoshan, Raphael, Ramu, Avner, Ringel, Israel
Format: Article
Language:English
Subjects:
Animals
Anthraquinones - chemical synthesis
Anthraquinones - pharmacology
Anthraquinones - therapeutic use
Antineoplastic Agents - chemical synthesis
Cisplatin - analogs & derivatives
Cisplatin - chemical synthesis
Cisplatin - pharmacology
Cisplatin - therapeutic use
Drug Screening Assays, Antitumor
Indicators and Reagents
Intercalating Agents - chemical synthesis
Intercalating Agents - pharmacology
Intercalating Agents - therapeutic use
Leukemia P388 - drug therapy
Mice
Mice, Inbred DBA
Molecular Structure
Structure-Activity Relationship
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Summary:A new series of complexes of the type cis-PtL2X2 [where L is a monodentate AQ-Y(CH2)nNH2 and L2 is a bidentate AQ-Y(CH2)nNH(CH2)2NH2; AQ = anthraquinone, X = Cl, I, Y = NH, O] in which anthraquinone intercalators are tethered to the cis-PtCl2 unit via an (aminoalkyl)amino, (oxyalkyl)amino, or polyethylene glycol (aminoethyl)amino linker chains was prepared and screened in vitro against P388 leukemia. In vivo toxicity studies were carried out on selected complexes. All complexes were characterized by means of elemental analysis, 195Pt NMR spectroscopy, and FTIR. The 1:1 Pt-intercalator complexes displayed much higher in vitro cytotoxic activities than the 1:2 Pt-intercalator complexes. The dichloride complexes were consistently more active than their diiodide counterparts. Among the 1:1 Pt-intercalator complexes those with the shorter linker chains (n = 2, 3) exhibited the highest cytotoxic activities. Three compounds, [[2-[[2-(anthraquinon-1- ylamino)ethyl]amino]ethyl]amine-N,N']dichloroplatinum(II), [[2-[[3-(anthraquinon-1-ylamino)propyl]amino]ethyl]amine- N,N']dichloroplatinum(II), and [[2-[[3-anthraquinon-1- yloxy)propyl]amino]ethyl]amine-N,N']dichloroplatinum(II), were as active in vitro as cisplatin (ED50 = 2-4 x 10(-7) M) while on a molar basis their acute in vivo toxicity was significantly lower than that of cisplatin. In vivo screening against P388 leukemia indicated that these complexes have activity comparable to cisplatin.
ISSN:0022-2623
1520-4804
DOI:10.1021/jm00105a063