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Photocytotoxic activity of a nitrosyl phthalocyanine ruthenium complex--a system capable of producing nitric oxide and singlet oxygen
Authors:Carneiro Zumira Aparecida  de Moraes Juliana Cristina Biazzotto  Rodrigues Fernando Postalli  de Lima Renata Galvão  Curti Carlos  da Rocha Zênis Novaes  Paulo Michele  Bendhack Lusiane Maria  Tedesco Antonio Claudio  Formiga André Luiz Barboza  da Silva Roberto Santana
Institution:
  • a Faculdade de Ciências Farmacêuticas de Ribeirão Preto, Universidade de São Paulo, Av. do Café s/n, 14040-903, Ribeirão Preto, SP, Brazil
  • b Universidade Federal da Bahia, Instituto de Química, Departamento de Química Geral e Inorgânica, Rua Barão de Geremoabo 147, Laboratório 208, sala 202 Ondina 41750003, Salvador, BA, Brazil
  • c Departamento de Química da Faculdade de Filosofia Ciências e Letras de Ribeirão Preto, Universidade de São Paulo, Av. dos Bandeirantes 3900, 14040-901, Ribeirão Preto, SP, Brazil
  • d Universidade Estadual Campinas, Instituto de Quimica, BR-13083970 Campinas, SP, Brazil
  • Abstract:The synthesis, structural aspects, pharmacological assays, and in vitro photoinduced cytotoxic properties of Ru(NO)(ONO)(pc)] (pc = phthalocyanine) are described. Its biological effect on the B16F10 cell line was studied in the presence and absence of visible light irradiation. At comparable irradiation levels, Ru(NO)(ONO)(pc)] was more effective than Ru(pc)] at inhibiting cell growth, suggesting that occurrence of nitric oxide release following singlet oxygen production upon light irradiation may be an important mechanism by which the nitrosyl ruthenium complex exhibits enhanced biological activity in cells. Following visible light activation, the Ru(NO)(ONO)(pc)] complex displayed increased potency in B16F10 cells upon modifications to the photoinduced dose; indeed, enhanced potency was detected when the nitrosyl ruthenium complex was encapsulated in a drug delivery system. The liposome containing the Ru(NO)(ONO)(pc)] complex was over 25% more active than the corresponding ruthenium complex in phosphate buffer solution. The activity of the complex was directly proportional to the ruthenium amount present inside the cell, as determined by inductively coupled plasma mass spectroscopy. Flow cytometry analysis revealed that the photocytotoxic activity was mainly due to apoptosis. Furthermore, the vasorelaxation induced by Ru(NO)(ONO)(pc)], proposed as NO carrier, was studied in rat isolated aorta. The observed vasodilation was concentration-dependent. Taken together, the present findings demonstrate that the Ru(NO)(ONO)(pc)] complex induces vascular relaxation and could be a potent anti-tumor agent. Nitric oxide release following singlet oxygen production upon visible light irradiation on a nitrosyl ruthenium complex produces two radicals and may elicit phototoxic responses that may find useful applications in photodynamic therapy.
    Keywords:Nitric oxide  Photocytotoxic activity  Nitrosyl ruthenium complex
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