Cobalt and Zinc Compounds Bearing 1,10-Phenanthroline-5,6-dione or 1,3,5-Triaza-7-phosphaadamantane Derivatives - Synthesis, Characterization, Cytotoxicity, and Cell Selectivity Studies

The compounds [mPTA][CoCl4] (1, mPTA = N-methyl-1,3,5-triaza-7-phosphaadamantane cation), [CoCl(H2O)(DION)(2)][BF4] (2, DION = 1,10-phenanthroline-5,6-dione), [Zn(DION)(2)]Cl-2 (3) and [ZnCl(O-PTA=O)(DION)][BF4] (4) were synthesized by reaction of CoCl2 with [mPTA]I or DION and ZnCl2 with DION or 1,3,5-triaza-7-phosphaadamantane-7-oxide (PTA=O) and DION, respectively. All complexes are water soluble and have been characterized by IR, far-IR, H-1, C-13 and P-31{H-1} NMR spectroscopy, ESI-MS, elemental analyses and single-crystal X-ray diffraction structural analysis (for 1). They were screened against the human tumour cell lines HCT116, HepG2 and MCF7. Complexes 2 and 3 exhibit the highest in vitro cytotoxicity and show lower cytotoxic activities in normal human fibroblast cell line than in HCT116 tumour cell line, which demonstrates their slight specificity for this type of tumour cell.

Syntheses, Molecular Structures, Electrochemical Behavior, Theoretical Study, and Antitumor Activities of Organotin(IV) Complexes Containing 1-(4-Chlorophenyl)-1-cyclopentanecarboxylato Ligands

The organotin(IV) compounds [Me2Sn(L)(2)] (1), [Et(2)sn(L)(2)] (2), [(Bu2Sn)-Bu-n(L)(2)] (3), [(n)Oct(2)Sn(L)(2)] (4), [Ph2Sn(L)(2)] (5), and [PhOSnL](6) (6) have been synthesized from the reactions of 1-(4-chlorophenyl)-1-cyclopentanecarboxylic acid (HL) with the corresponding diorganotin(IV) oxide or dichloride. They were characterized by IR and multinuclear NMR spectroscopies, elemental analysis, cyclic voltammetry, and, for 2, 3, 4 and 6, single crystal X-ray diffraction analysis. While 1-5 are mononuclear diorganotin (IV) compounds, the X-ray diffraction of 6 discloses a hexameric drumlike structure with a prismatic Sn6O6 core. All these complexes undergo irreversible reductions and were screened for their in vitro antitumor activities toward HL-60, BGC-823, Bel-7402, and KB human cancer cell lines. Within the mononuclear compounds, the most active ones (3, 5) are easiest to reduce (least cathodic reduction potentials), while the least active ones (1, 4) are the most difficult to reduce. Structural rearrangements (i.e., Sn-O bond cleavages and trans-to-cis isomerization) induced by reduction, which eventually can favor the bioactivity, are disclosed by theoretical/electrochemical studies.

Insights into the mechanims underlyng the antiproliferative potential of a Co(II) coordination compound bearing 1,10-Phenanthroline-5,6-Dione: DNA and protein interaction studies

The very high antiproliferative activity of [Co(Cl)(H2O)(phendione)(2)][BF4] (phendione is 1,10-phenanthroline-5,6-dione) against three human tumor cell lines (half-maximal inhibitory concentration below 1 mu M) and its slight selectivity for the colorectal tumor cell line compared with healthy human fibroblasts led us to explore the mechanisms of action underlying this promising antitumor potential. As previously shown by our group, this complex induces cell cycle arrest in S phase and subsequent cell death by apoptosis and it also reduces the expression of proteins typically upregulated in tumors. In the present work, we demonstrate that [Co(Cl)(phendione)(2)(H2O)][BF4] (1) does not reduce the viability of nontumorigenic breast epithelial cells by more than 85 % at 1 mu M, (2) promotes the upregulation of proapoptotic Bax and cell-cycle-related p21, and (3) induces release of lactate dehydrogenase, which is partially reversed by ursodeoxycholic acid. DNA interaction studies were performed to uncover the genotoxicity of the complex and demonstrate that even though it displays K (b) (+/- A standard error of the mean) of (3.48 +/- A 0.03) x 10(5) M-1 and is able to produce double-strand breaks in a concentration-dependent manner, it does not exert any clastogenic effect ex vivo, ruling out DNA as a major cellular target for the complex. Steady-state and time-resolved fluorescence spectroscopy studies are indicative of a strong and specific interaction of the complex with human serum albumin, involving one binding site, at a distance of approximately 1.5 nm for the Trp214 indole side chain with log K (b) similar to 4.7, thus suggesting that this complex can be efficiently transported by albumin in the blood plasma.

Greener Selective Cycloalkane Oxidations with Hydrogen Peroxide Catalyzed by Copper-5-(4-pyridyl)tetrazolate Metal-Organic Frameworks

Microwave assisted synthesis of the Cu(I) compound [Cu(µ4-4-ptz)]n [1, 4-ptz = 5-(4-pyridyl)tetrazolate] has been performed by employing a relatively easy method and within a shorter period of time compared to its sister compounds. The syntheses of the Cu(II) compounds [Cu3(µ3-4-ptz)4(µ2-N3)2(DMF)2]n∙(DMF)2n (2) and [Cu(µ2-4-ptz)2(H2O)2]n (3) using a similar method were reported previously by us. MOFs 1-3 revealed high catalytic activity toward oxidation of cyclic alkanes (cyclopentane, -hexane and -octane) with aqueous hydrogen peroxide, under very mild conditions (at room temperature), without any added solvent or additive. The most efficient system (2/H2O2) showed, for the oxidation of cyclohexane, a turnover number (TON) of 396 (TOF of 40 h−1), with an overall product yield (cyclohexanol and cyclohexanone) of 40% relative to the substrate. Moreover, the heterogeneous catalytic systems 1–3 allowed an easy catalyst recovery and reuse, at least for four consecutive cycles, maintaining ca. 90% of the initial high activity and concomitant high selectivity.

Síntese de precursores de ligando do tipo 5-aril-2-iminopirrole e sua aplicação na preparação de complexos de níquel

O trabalho apresentado nesta dissertação centrou-se na síntese e caracterização de novos precursores de ligandos do tipo iminopirrolilo, usando como molécula de partida a 2-fenil-1-pirrolina. Estes ligandos foram posteriormente usados em tentativas de síntese de complexos de Ni(II). Em termos experimentais, este trabalho foi iniciado pelo estudo da síntese do 2- fenilpirrole a partir da 2-fenil-1-pirrolina, na tentativa de obter um produto puro, através de um processo competitivo em termos de eficiência e custo em relação aos descritos anteriormente pelo grupo de trabalho e pela literatura. Numa segunda fase, estudou-se a síntese de dois novos precursores de ligandos iminopirrolilo e, por fim, tentou-se sintetizar dois novos complexos de Ni(II) com base nos referidos ligandos, com vista ao seu uso como catalisadores de polimerização de olefinas. O Capítulo 1 apresenta uma introdução ao desenvolvimento dos complexos de metais de transição como catalisadores de polimerização de olefinas, dando-se ênfase especial aos catalisadores de níquel contendo ligandos α-diimina, fenoxi-imina, anilitropona e iminopirrolilo. Focam-se ainda os métodos de síntese de pirroles substituídos na posição 2, devido à importância que apresentam para os objectivos deste trabalho. No Capítulo 2 estuda-se a reacção de desidrogenação catalítica de 2-fenil-1-pirrolina a 2-fenilpirrole, catalisada por paládio suportado em carvão ou alumina activados. Posteriormente descreve-se a reacção de formilação do 2-fenilpirrole que origina o novo composto 5-fenil-2-formilpirrole. Este é transformado em novos precursores de ligando do tipo iminopirrolilo, mais especificamente 2-arilimino-5-fenilpirrolilo, por condensação com a dimetil- e diisopropilanilina. No Capítulo 3 discute-se as tentativas de síntese de novos complexos de Ni(II) contendo os ligandos iminopirrolilo sintetizados, a partir da reacção dos correspondentes sais de sódio com o complexo [NiCl(Ph)(PPh3)2]. O Capítulo 4 apresenta as conclusões gerais e o Capítulo 5 os detalhes experimentais, as sínteses e as caracterizações dos ligandos e dos complexos.

Manual para a elaboração de dissertações

1. INTRODUÇÃO; 2. PROCEDIMENTOS DE ENTREGA DA DISSERTAÇÃO; 3. ESTRUTURA DA DISSERTAÇÃO; 4. FORMATAÇÃO; 5. CITAÇÕES; 6. CONCLUSÃO; BIBLIOGRAFIA; APÊNDICES