Resumo
Background: Ruthenium-based anti-cancer compounds are proposed as viable alternatives that might circumvent the disadvantages of platinum-based drugs, the only metallodrugs in clinical use for chemotherapy. Organometallic complexes in particular hold great potential as alternative therapeutic agents since their cytotoxicity involves different modes of action and present reduced toxicity profiles. Objective: During the last few years our research group has been reporting on a series of organometallic ruthenium(II)-cyclopentadienyl complexes with important cytotoxicity against several cancer cell lines, surpassing cisplatin in activity. We report herein preliminary in vivo studies with one representative compound of this family, with exceptional activity against several human cancer cell lines, including the glycolytic and highly metastatic MDAMB231 cell line used in this study. Method: The anti-tumor activity of our compound was studied in vivo on N:NIH(S)II-nu/nu nude female mice bearing triple negative breast cancer (TNBC) orthotopic tumors. Administration of 2.5 mg/kg/day during ten days caused cell death mostly by necrosiscontrols.(in vitro and in vivo), inducing tumor growth suppression of about 50% in treated animals when compared to Results: The most remarkable result supporting the effectiveness and potential of this drug was the absence of metastases in the main organs of treated animals, whileanalysis.metastases were present in the lungs of all control mice, as revealed by histopathological and immunohistochemical Conclusion: These in vivo studies suggest a dual effect for our drug not only by suppressing growth at the primary tumor tissue but also by inhibiting its metastatic behavior. Altogether, these results represent a benchmark and a solid starting point for future studies.
Idioma original | ???core.languages.en_GB??? |
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Páginas (de-até) | 126-136 |
Número de páginas | 11 |
Revista | Anti-Cancer Agents in Medicinal Chemistry |
Volume | 17 |
Número de emissão | 1 |
DOIs | |
Estado da publicação | ???researchoutput.status.published??? - 2017 |