Is the Aromatic Fragment of Piano‐Stool Ruthenium Compounds an Essential Feature for Anticancer Activity? The Development of New Ru II ‐[9]aneS 3 Analogues

Is the Aromatic Fragment of Piano‐Stool Ruthenium Compounds an Essential Feature for Anticancer Activity? The Development of New Ru II ‐[9]aneS 3 Analogues

New half‐sandwich Ru II ‐[9]aneS 3 complexes ([9]aneS 3 = 1,4,7‐trithiacyclononane), namely [RuCl 2 (PTA)([9]aneS 3 )] ( 4 ), [RuCl(PTA) 2 ([9]aneS 3 )][OTf] ( 5 ), [RuCl(en)([9]aneS 3 )][OTf] ( 6 ), [RuCl(enac)([9]aneS 3 )][OTf] ( 7 ), [RuCl(bipy)([9]aneS 3 )][OTf] ( 8 ), and [Ru(dmso‐S)(bipy)([9]a...

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Bibliographic Details
Published in:European journal of inorganic chemistry Vol. 2005; no. 17; pp. 3423 - 3434
Main Authors: Serli, Barbara, Zangrando, Ennio, Gianferrara, Teresa, Scolaro, Claudine, Dyson, Paul J., Bergamo, Alberta, Alessio, Enzo
Format: Journal Article
Language:English
Published: 01-09-2005
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Summary:New half‐sandwich Ru II ‐[9]aneS 3 complexes ([9]aneS 3 = 1,4,7‐trithiacyclononane), namely [RuCl 2 (PTA)([9]aneS 3 )] ( 4 ), [RuCl(PTA) 2 ([9]aneS 3 )][OTf] ( 5 ), [RuCl(en)([9]aneS 3 )][OTf] ( 6 ), [RuCl(enac)([9]aneS 3 )][OTf] ( 7 ), [RuCl(bipy)([9]aneS 3 )][OTf] ( 8 ), and [Ru(dmso‐S)(bipy)([9]aneS 3 )][OTf] 2 ( 9 ) [PTA = 1,3,5‐triaza‐7‐phosphaadamantane; enac = 1,2‐bis(isopropyleneimino)ethane; OTf = CF 3 SO 3 – ] were prepared from Ru‐[9]aneS 3 –dmso precursors and structurally characterized, both in solution and in the solid state by X‐ray crystallography. Some of them are analogs of known cytotoxic organometallic Ru II ‐(η 6 ‐arene) and Ru II ‐(η 5 ‐cyclopentadienyl) compounds, in which the aromatic fragment is replaced by the sulfur macrocycle 1,4,7‐trithiacyclononane, while the rest of the coordination sphere is left unchanged. Similarly to the aromatic analogs for which data are available, in aqueous solution the Ru‐[9]aneS 3 complexes (with the exception of 5 ) hydrolyze a chloride (or a dmso in the case of 9 ) to give the corresponding aquo species. This process is rapidly reversed in the presence of free chloride, and coordination of phosphate is likely to occur to the aquo species in phosphate buffered solutions at physiological pH. Preliminary in vitro tests performed on complexes 4 – 6 against the mouse adenocarcinoma cancer cell line (TS/A) and the human mammary normal cell line (HBL‐100) showed that, in general, the Ru‐[9]aneS 3 compounds have a cytotoxicity comparable to that of the corresponding organometallic analogs. These results suggest that the aromatic fragment of the piano‐stool Ru II compounds is not an essential feature for the in vitro anticancer activity, and it might be effectively replaced by another face‐capping ligand with a low steric demand, such as [9]aneS 3 . (© Wiley‐VCH Verlag GmbH & Co. KGaA, 69451 Weinheim, Germany, 2005)
ISSN:1434-1948
1099-0682
DOI:10.1002/ejic.200500210