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Characterization of the anti tumoral activity of the thiosemicarbazones derived from N(4)-methyl-tolyl-2acetylpyridine And 2-pyridinoformamide and its metal complex: evaluation of the radiopharmaceutical potential; Caracterizacao da atividade antitumoral das tiossemicarbazonas derivadas de N(4)-metil-toluil-2-acetilpiridina e 2-piridinoformamida e seus complexos metalicos: avaliacao do potencial radiofarmaceutico

Abstract

Thiosemicarbazones have attracted great pharmacological interest because of their biological properties, such as cytotoxic activity against multiple strains of human tumors. The most studied compounds are pyridine-based because of their resemblance to pyridoxal metabolites that attach to co-enzyme B{sub 6}-dependant enzymes. This work aimed the characterization of the anti tumoral effect of N(4)-methyl-tolyl-2-acetylpyridine and 2-pyridinoformamide-derived thiosemicarbazones and the development of a radiopharmaceutical based on a thiosemicarbazone metal complex for positron emission tomography. In the first phase of this study were synthesized twenty-one thiosemicarbazones, derived from N(4)methyl-2 acetylpyridine and 2-pyridine formamide, as well as their metal complexes (Sn, Ga and Cu). Their cytotoxic potential were evaluated against brain and breast tumor cells in vitro. Our results showed all of them presented powerful cytotoxic and antiproliferative activities against glioblastoma multiform and breast adenocarcinoma at very low concentrations (nanomolar range). Morphological alterations characteristic of apoptosis, such as cell shrinkage, chromatin condensation were observed. Copper chloride was used as control and has presented IC50 at millimolar range suggesting that copper complexation with thiosemicarbazone significantly increases (more than 1 million) the anti tumoral effect of this metal. Due to the potent anti tumoral activity of N(4)-methyl-tolyl-2-acetylpyridine derived thiosemicarbazones and the excellent properties of {sup 64}Cu  More>>
Publication Date:
Jul 01, 2008
Product Type:
Thesis/Dissertation
Report Number:
INIS-BR-5510
Resource Relation:
Other Information: TH: Diss. (M.Sc.); 84 refs., 63 figs., 12 tabs
Subject:
38 RADIATION CHEMISTRY, RADIOCHEMISTRY, AND NUCLEAR CHEMISTRY; ANTI-INFECTIVE AGENTS; ANTIMITOTIC DRUGS; ASCITES TUMOR CELLS; CARBAZONES; DYNAMIC FUNCTION STUDIES; NEOPLASMS; NUCLEAR MEDICINE; POSITRON CAMERAS; POSITRON COMPUTED TOMOGRAPHY; RADIOISOTOPES; RADIOPHARMACEUTICALS; TUMOR CELLS
OSTI ID:
21203097
Research Organizations:
Centro de Desenvolvimento da Tecnologia Nuclear (CDTN/CNEN-MG), Belo Horizonte, MG (Brazil).Programa de Pos-Graduacao em Ciencia e Tecnologia das Radiagcoes, Minerais e Materiais
Country of Origin:
Brazil
Language:
Portuguese
Other Identifying Numbers:
TRN: BR09V2502073555
Availability:
Available from INIS in electronic form
Submitting Site:
BRN
Size:
172 pages
Announcement Date:
Aug 21, 2009

Citation Formats

Silva, Paulo Roberto Ornelas da. Characterization of the anti tumoral activity of the thiosemicarbazones derived from N(4)-methyl-tolyl-2acetylpyridine And 2-pyridinoformamide and its metal complex: evaluation of the radiopharmaceutical potential; Caracterizacao da atividade antitumoral das tiossemicarbazonas derivadas de N(4)-metil-toluil-2-acetilpiridina e 2-piridinoformamida e seus complexos metalicos: avaliacao do potencial radiofarmaceutico. Brazil: N. p., 2008. Web.
Silva, Paulo Roberto Ornelas da. Characterization of the anti tumoral activity of the thiosemicarbazones derived from N(4)-methyl-tolyl-2acetylpyridine And 2-pyridinoformamide and its metal complex: evaluation of the radiopharmaceutical potential; Caracterizacao da atividade antitumoral das tiossemicarbazonas derivadas de N(4)-metil-toluil-2-acetilpiridina e 2-piridinoformamida e seus complexos metalicos: avaliacao do potencial radiofarmaceutico. Brazil.
Silva, Paulo Roberto Ornelas da. 2008. "Characterization of the anti tumoral activity of the thiosemicarbazones derived from N(4)-methyl-tolyl-2acetylpyridine And 2-pyridinoformamide and its metal complex: evaluation of the radiopharmaceutical potential; Caracterizacao da atividade antitumoral das tiossemicarbazonas derivadas de N(4)-metil-toluil-2-acetilpiridina e 2-piridinoformamida e seus complexos metalicos: avaliacao do potencial radiofarmaceutico." Brazil.
@misc{etde_21203097,
title = {Characterization of the anti tumoral activity of the thiosemicarbazones derived from N(4)-methyl-tolyl-2acetylpyridine And 2-pyridinoformamide and its metal complex: evaluation of the radiopharmaceutical potential; Caracterizacao da atividade antitumoral das tiossemicarbazonas derivadas de N(4)-metil-toluil-2-acetilpiridina e 2-piridinoformamida e seus complexos metalicos: avaliacao do potencial radiofarmaceutico}
author = {Silva, Paulo Roberto Ornelas da}
abstractNote = {Thiosemicarbazones have attracted great pharmacological interest because of their biological properties, such as cytotoxic activity against multiple strains of human tumors. The most studied compounds are pyridine-based because of their resemblance to pyridoxal metabolites that attach to co-enzyme B{sub 6}-dependant enzymes. This work aimed the characterization of the anti tumoral effect of N(4)-methyl-tolyl-2-acetylpyridine and 2-pyridinoformamide-derived thiosemicarbazones and the development of a radiopharmaceutical based on a thiosemicarbazone metal complex for positron emission tomography. In the first phase of this study were synthesized twenty-one thiosemicarbazones, derived from N(4)methyl-2 acetylpyridine and 2-pyridine formamide, as well as their metal complexes (Sn, Ga and Cu). Their cytotoxic potential were evaluated against brain and breast tumor cells in vitro. Our results showed all of them presented powerful cytotoxic and antiproliferative activities against glioblastoma multiform and breast adenocarcinoma at very low concentrations (nanomolar range). Morphological alterations characteristic of apoptosis, such as cell shrinkage, chromatin condensation were observed. Copper chloride was used as control and has presented IC50 at millimolar range suggesting that copper complexation with thiosemicarbazone significantly increases (more than 1 million) the anti tumoral effect of this metal. Due to the potent anti tumoral activity of N(4)-methyl-tolyl-2-acetylpyridine derived thiosemicarbazones and the excellent properties of {sup 64}Cu (T{sub 1/2} = 12.7 hours, {beta}{sup +}, {beta}{sup -}, and EC decay), at the second part for this work it was developed a new imaging agent (radiopharmaceutical) for tumor detection by positron emission tomography (PET). The radiopharmaceuticals were produced in the nuclear reactor TRIGA-IPR-R1 from CDTN, via neutron capture reaction {sup 63}Cu (n,{gamma}) {sup 64}Cu, of the copper complex N(4)-ortho-toluyl-2-acetylpyridine thiosemicarbazone (Culac). The induced specific activity was found to be 5.55 MBq /mg. After irradiation Culac samples were analyzed by the absorption of infrared spectroscopy (IR) to assess the structural integrity. The irradiated compound kept its structural integrity. The maintenance of {sup 64}Culac biological activity was also evaluated by MTT assay on RT2 (wild p53), T98 (mutant p53), MCF-7 (wild p53) and CAE cells (wild p53). The results showed that {sup 64}Culac kept its potent anti tumoral activity against all treated cells presenting IC50 values at nanomolar range. {sup 64}Culac biodistribution studies after intravenous injection in mice bearing Erlich tumor implanted in the paw, showed significant uptake in the tumor paw (tumor/skeletal muscle ratio 6.55), 240 minutes after administration. Histopathological studies have shown mild hepatotoxicity 144 hours (6 days) after intravenous administration of 308 mg/kg of Culac. However, no lethality, behavioural, or feeding changes were observed at this dose. Our results demonstrate that the complex of copper-64 N(4)-ortho-toluyl-2-acetylpyridine thiosemicarbazone ({sup 64}Culac) is a promising radiopharmaceutical for detection of solid tumors by positron emission tomography (PET). (author)}
place = {Brazil}
year = {2008}
month = {Jul}
}