Striking Difference in Antiproliferative Activity of Ruthenium- and Osmium-Nitrosyl Complexes with Azole Heterocycles

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Striking Difference in Antiproliferative Activity of Ruthenium- and Osmium-Nitrosyl Complexes with Azole Heterocycles

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作者：Gabriel E. B眉chel ; Anatolie Gavriluta ; Maria Novak ; Samuel M. Meier ; Michael A. Jakupec ; Olesea Cuzan ; Constantin Turta ; Jean-Bernard Tommasino ; Erwann Jeanneau ; Ghenadie Novitchi ; Dominique Luneau ; Vladimir B. Arion
刊名：Inorganic Chemistry
出版年：2013
出版时间：June 3, 2013
年：2013
卷：52
期：11
页码：6273-6285
全文大小：506K
年卷期：v.52,no.11(June 3, 2013)
ISSN：1520-510X

文摘

Ruthenium nitrosyl complexes of the general formulas (cation)⁺[cis-RuCl₄(NO)(Hazole)]^{鈭?/sup>, where (cation)⁺ = (H₂ind)⁺, Hazole = 1H-indazole (Hind) (1c), (cation)⁺ = (H₂pz)⁺, Hazole = 1H-pyrazole (Hpz) (2c), (cation)⁺ = (H₂bzim)⁺, Hazole = 1H-benzimidazole (Hbzim) (3c), (cation)⁺ = (H₂im)⁺, Hazole = 1H-imidazole (Him) (4c) and (cation)⁺[trans-RuCl₄(NO)(Hazole)]^{鈭?/sup>, where (cation)⁺ = (H₂ind)⁺, Hazole = 1H-indazole (1t), (cation)⁺ = (H₂pz)⁺, Hazole = 1H-pyrazole (2t), as well as osmium analogues of the general formulas (cation)⁺[cis-OsCl₄(NO)(Hazole)]^{鈭?/sup>, where (cation)⁺ = (n-Bu₄N)⁺, Hazole =1H-indazole (5c), 1H-pyrazole (6c), 1H-benzimidazole (7c), 1H-imidazole (8c), (cation)⁺ = Na⁺; Hazole =1H-indazole (9c), 1H-benzimidazole (10c), (cation)⁺ = (H₂ind)⁺, Hazole = 1H-indazole (11c), (cation)⁺ = H₂pz⁺, Hazole = 1H-pyrazole (12c), (cation)⁺ = (H₂im)⁺, Hazole = 1H-imidazole (13c), and (cation)⁺[trans-OsCl₄(NO)(Hazole)]^{鈭?/sup>, where (cation)⁺ = n-Bu₄N⁺, Hazole = 1H-indazole (5t), 1H-pyrazole (6t), (cation)⁺ = Na⁺, Hazole = 1H-indazole (9t), (cation)⁺ = (H₂ind)⁺, Hazole = 1H-indazole (11t), (cation)⁺ = (H₂pz)⁺, Hazole = 1H-pyrazole (12t), have been synthesized. The compounds have been comprehensively characterized by elemental analysis, ESI mass spectrometry, spectroscopic techniques (IR, UV鈥搗is, 1D and 2D NMR) and X-ray crystallography (1c路CHCl₃, 1t路CHCl₃, 2t, 3c, 6c, 6t, 8c). The antiproliferative activity of water-soluble compounds (1c, 1t, 3c, 4c and 9c, 9t, 10c, 11c, 11t, 12c, 12t, 13c) in the human cancer cell lines A549 (nonsmall cell lung carcinoma), CH1 (ovarian carcinoma), and SW480 (colon adenocarcinoma) has been assayed. The effects of metal (Ru vs Os), cis/trans isomerism, and azole heterocycle identity on cytotoxic potency and cell line selectivity have been elucidated. Ruthenium complexes (1c, 1t, 3c, and 4c) yielded IC₅₀ values in the low micromolar concentration range. In contrast to most pairs of analogous ruthenium and osmium complexes known, they turned out to be considerably more cytotoxic than chemically related osmium complexes (9c, 9t, 10c, 11c, 11t, 12c, 12t, 13c). The IC₅₀ values of Os/Ru homologs differ by factors (Os/Ru) of up to 110 and 410 in CH1 and SW480 cells, respectively. ESI-MS studies revealed that ascorbic acid may activate the ruthenium complexes leading to hydrolysis of one M鈥揅l bond, whereas the osmium analogues tend to be inert. The interaction with myoglobin suggests nonselective adduct formation; i.e., proteins may act as carriers for these compounds.}}}}