Synthesis, characterization and in vitro biological evaluation of [Ru(eta(6)-arene)(N,N)Cl] PF6 compounds using the natural products arenes methylisoeugenol and anethole
Author
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Delgado, Ricardo
Author
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Galdámez Silva, Antonio
Author
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Villena, Joan
Author
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Reveco, Patricio
Author
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Thomet, Franz A.
Admission date
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2015-08-31T20:01:39Z
Available date
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2015-08-31T20:01:39Z
Publication date
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2015
Cita de ítem
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Journal of Organometallic Chemistry 782 (2015) 131-137
en_US
Identifier
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DOI: 10.1016/j.jorganchem.2014.09.005
Identifier
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https://repositorio.uchile.cl/handle/2250/133327
General note
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Artículo de publicación ISI
en_US
Abstract
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Five new organometallic Ru(II) compounds (VI-X) with the general formula [Ru(eta(6)-arene)(N,N)CI]PF6, where arene-N,N correspond to methylisoeugenol-bipyridine (VI); anethole-bipyridine (VII); methylisoeugenol-ethylenediamine (VIII); anethole-ethylenediamine (IX) and methylisoeugenol-1,2-diaminobenzene (X), have been synthesized, fully characterized and biologically evaluated in vitro. The reaction conditions based on the reduction of [Ru(1,5-COD)Cl-2](n) in situ with methyleugenol and estragole, which are natural ligands, induced an alkene isomerization on the allylic substituent of coordinated arenes. The Ru(II)-arene bond formation and isomerization of the C=C bond on the allyl substituent was confirmed using 1H NMR spectroscopy; this result was validated for compound VIII by X-ray diffraction. An XRD analysis revealed the presence of both enantiomers of the complex in the single-crystal. Compounds IX and X exhibited a better cytotoxic activity in vitro than carboplatin, which is a commercial drug, against three human tumor cell lines (MCF-7, PC-3 and HT-29).
Synthesis, characterization and in vitro biological evaluation of [Ru(eta(6)-arene)(N,N)Cl] PF6 compounds using the natural products arenes methylisoeugenol and anethole