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Previous issue date: 2010-04-05 / In this thesis complexes of general formula: [Ru(NS)(bipy)(PP)]PF6 (NS = 2-mercaptopyridine, 2-mercaptopyrimidine, 4,6-dimethyl-2- mercaptopyrimidine and PP = dppf, dppp, dppe); [Ru(pic)(bipy)(PP)]PF6 (pic = picolinate; PP = dppf, dppp, dppe and dppm), [RuCl(bCN)(bipy)(PP)]PF6 (bCN = benzonitrile; PP = dppf and dppe), and [RuCl(bCN)(NN)(dppb)]PF6 (NN = bipy, Mebipy and phen), were synthesised from the precursor complexes cis- [RuCl2(NN)(PP)] and characterized by the usual techniques: 1H and 31P{1H} NMR, IR, UV-Vis, molar conductimetry, elemental analysis, cyclic and differential pulse voltammetry and single-crystal X-ray diffraction (except for the compounds [Ru(pic)(bipy)(dppp)]PF6, [Ru(pic)(bipy)(dppm)]PF6 and [RuCl(bCN)(Mebipy)(dppb)]PF6, which suitable single crystal were not obtained). The 31P{1H} NMR spectras of the new compounds showed that the phosphorus atoms were more deshielded than in the correspondent precursor. The E1/2 values of the complexes containing the ligands NS, pic and bCN were higher than those observed in the precursor complexes. The complexes containing the ligand dppf presented two redox process, which were assigned to the redox pairs FeII/FeIII and RuII/RuIII respectively, according to the results of the kinetics experiments monitored by differential pulse voltammetry and 31P{1H} NMR techniques. The molar conductimetry and elemental analysis assays corroborated the proposed formula and the single-crystal X-ray diffraction study of these complexes confirmed their structures. The νCN in the complexes [RuCl(bCN)(NN)(PP)]PF6 were higher (~+8 cm-1) than that observed in the free ligand (2229 cm-1). Also, it was avaluated in vitro antitumor activity of some of the compounds synthesised herein against mammary cancer cell line (MDA-MB-231), murine sarcoma, as well as against M. tuberculosis (H37Rv); some of them presented high activity. / Neste trabalho foram sintetizados os complexos de fórmula: [Ru(NS)(bipy)(PP)]PF6 (NS = 2-mercaptopiridina, 2-mercaptopirimidina, 4,6- dimetil-2-mercaptopirimidina e PP = dppf, dppp, dppe); [Ru(pic)(bipy)(PP)]PF6 (PP = dppf, dppp, dppe e dppm), [RuCl(bCN)(bipy)(PP)]PF6 (bCN = benzonitrila; PP = dppf e dppe), e [RuCl(bCN)(NN)(dppb)]PF6 (NN = bipy, Mebipy e phen) a partir dos complexos precursores de fórmula cis- [RuCl2(NN)(PP)], e foram caracterizados pelas técnicas de RMN de 1H e 31P{1H}, IV, UV-Vis, condutância molar, análise elementar, voltametrias cíclica e de pulso diferencial e por difração de raios-X de monocristal (à exceção dos compostos [Ru(pic)(bipy)(dppp)]PF6, [Ru(pic)(bipy)(dppm)]PF6, [RuCl(bCN)(Mebipy)(dppb)]PF6, dos quais não se obteve cristais adequados para estudado por difração de raios-X). Os espectros de RMN de 31P{1H} mostraram que ocorre a desblindagem dos átomos de fósforo causada pela coordenação dos ligantes NS, pic e bCN. Os complexos sintetizados apresentaram valores de E1/2 maiores que seus correspondentes precursores, e aqueles contendo a bifosfina dppf apresentaram dois processos redox, que através de experimentos de cinética realizados por voltametria de pulso diferencial e RMN de 31P{1H} puderam ser atribuídos aos pares FeII/FeIII e RuII/RuIII, respectivamente. As medidas de condutância molar e as de análise elementar corroboraram as fórmulas propostas e o estudo dos cristais resolvidos por difração de raios-X confirmaram as estruturas esperadas. Os valores de νCN nos complexos [RuCl(bCN)(NN)(PP)]PF6 foram maiores (~+8 cm-1) que o observado no ligante bCN livre (2229 cm-1). Alguns dos complexos sintetizados neste trabalho também foram avaliados in vitro como agentes antitumorais contra a linhagem de células de câncer de mama MDA-MB-231, sarcoma murino e também como anti-M. tuberculosis (H37Rv); alguns deles mostraram bons resultados.
| Identifer | oai:union.ndltd.org:IBICT/oai:repositorio.ufscar.br:ufscar/6465 |
| Date | 05 April 2010 |
| Creators | Lima, Benedicto Augusto Vieira |
| Contributors | Batista, Alzir Azevedo |
| Publisher | Universidade Federal de São Carlos, Programa de Pós-graduação em Química, UFSCar, BR |
| Source Sets | IBICT Brazilian ETDs |
| Language | Portuguese |
| Detected Language | English |
| Type | info:eu-repo/semantics/publishedVersion, info:eu-repo/semantics/masterThesis |
| Format | application/pdf |
| Source | reponame:Repositório Institucional da UFSCAR, instname:Universidade Federal de São Carlos, instacron:UFSCAR |
| Rights | info:eu-repo/semantics/openAccess |
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