Your search keyword '"G. Cantinho"' showing total 4 results

1. Novel 3+1 mixed-ligand Technetium-99m complexes carrying dipeptides as monodentate ligands.

Author

Fernandes C, Patrício L, Moreira R, Cantinho G, Pena H, Campello PC, and Santos I

Subjects

Animals, Dipeptides chemistry, Drug Stability, Female, Isotope Labeling, Ligands, Metabolic Clearance Rate, Mice, Organ Specificity, Radiopharmaceuticals chemical synthesis, Radiopharmaceuticals pharmacokinetics, Technetium chemistry, Tissue Distribution, Dipeptides pharmacokinetics, Technetium pharmacokinetics

Abstract

Novel mixed ligand oxotechnetium complexes of the type [99mTcO(SSS)(SR)], in which the SR monodentate ligand is derived from dipeptides gly-gly, phe-gly and ala-gly, have been synthesized. These complexes, which have a molecular weight above 300, a lipophilic moiety, [TcO(SSS)]+, and an ionizable group separated from the lipophilic moiety by a spacer, have been obtained in 70-95% radiochemical yield. These compounds were prepared using 99mTc-tartrate as the precursor and Sn2+ as the reducing agent. The identity of the [99mTcO(SSS)(SR)] complexes has been established by HPLC comparison with the analogous oxorhenium complexes. The nature of the monodentate co-ligand strongly affects the stability of the 99mTc-complexes and their biodistribution. Complex 3b is the most stable in vitro presenting the highest blood clearance, a high liver uptake and a selective hepatobiliary excretion (54.5% ID at 15 min post-injection, and 69.3% ID at 60 min post injection). The results obtained show that 3b have reasonable stability and in vivo properties that may be useful for peptide labeling.

Published

2004

2. N-Carboxyalkyl derivatives of 3-hydroxy-4-pyridinones: synthesis, complexation with Fe(III), Al(III) and Ga(III) and in vivo evaluation.

Author

Santos MA, Gil M, Marques S, Gano L, Cantinho G, and Chaves S

Subjects

Animals, Chelation Therapy, Female, Hydrogen-Ion Concentration, Kinetics, Ligands, Mice, Organometallic Compounds metabolism, Protons, Pyridones chemical synthesis, Thermodynamics, Titrimetry, Aluminum metabolism, Gallium metabolism, Iron metabolism, Pyridones metabolism, Pyridones pharmacokinetics

Abstract

A set of three N-carboxyalkyl 3-hydroxy-4-pyridinones has been studied as bidentate M(III) chelators (M=Fe, Al, Ga), with potential for oral administration. After preparation of the ligands, their protonation constants (log K(i)) and the stability constants of their metal complexes have been determined. The distribution coefficients of these compounds, between 1-octanol and Tris buffer pH 7.4, were measured. The effect of these compounds on the biodistribution of 67Ga-citrate loaded rats was investigated and compared with that of the administered 67Ga-complexes. Results indicated that, among these chelating agents, the N-carboxyethyl derivative has the highest affinity towards this set of metal ions, irrespective of the metal, and that it could even compete with transferrin, the main Fe-plasma protein. The binding affinity and the hydrophilic character decrease with the increase in the size of the alkylic chain. The biological assays indicate that the complex formation in vivo is characterized by a high kinetics and thermodynamic stability, suggesting a competition with the transferrin. All the ligands were found to enhance the excretion of the gallium. Noteworthy is the observed Ga bone fixation, mostly with the ethyl derivative, thus suggesting the potential use of the complex as a bone seeking agent.

Published

2002

3. Synthesis, chelating properties towards gallium and biological evaluation of two N-substituted 3-hydroxy-4-pyridinones.

Author

Santos MA, Grazina R, Neto AQ, Cantinho G, Gano L, and Patrício L

Subjects

Animals, Chelating Agents pharmacology, Citrates pharmacokinetics, Female, Gallium chemistry, Gallium pharmacokinetics, Gallium Radioisotopes pharmacokinetics, Hydrogen-Ion Concentration, Ligands, Mice, Models, Chemical, Octanols metabolism, Propionates pharmacology, Propylamines pharmacology, Pyridones pharmacology, Time Factors, Tissue Distribution, Water metabolism, Gallium metabolism, Propionates metabolism, Propylamines metabolism, Pyridones chemistry, Pyridones metabolism

Abstract

Two N-substituted 3-hydroxy-4-pyridinones (1-(3'-aminopropyl)-3-hydroxy-2-methyl-4-pyridinone (L1) and 1-(2'-carboxyethyl)-3-hydroxy-2-methyl-4-pyridinone (L2)) were prepared through one- and three-step reactions, respectively. The pKa values of the ligands and the stability constants of their Ga(III) complexes have been determined. Both the complexes are strongly coordinated to three (O,O) hydroxypyridonate moieties. There is a clear effect of the N-substituents in the lipophilic-hydrophilic balance and in the Ga(III) binding interaction; the acid derivative (L2) has lower lipophilicity but higher chelating strength than the amine derivative (L1). Both chelators are shown to interfere in the typical biological behavior of 67Ga-citrate in mice: L1 enhanced the urinary excretion leading to an increased 67Ga removal from the soft tissue, while L2 induced a lower blood clearance with a pronounced bone uptake mainly at 48 h after injection, thus suggesting that the 67Ga-L2 complex could have potential interest as a bone imaging agent.

Published

2000

4. Human polyclonal immunoglobulin labelled with technetium-99m via NHS-MAG3: a comparison of radiochemical behavior and biological efficacy with other labelling methods.

Author

Gano L, Patrício L, Marques E, Cantinho G, Pena H, Martins T, and Hnatowich DJ

Subjects

Animals, Chromatography, High Pressure Liquid, Electrophoresis, Polyacrylamide Gel, Humans, Imidoesters pharmacology, Isotope Labeling methods, Male, Mercaptoethanol pharmacology, Mice, Radiochemistry, Sulfhydryl Compounds isolation & purification, Technetium, Tin pharmacology, Immunoglobulins metabolism, Staphylococcal Infections metabolism, Technetium Tc 99m Mertiatide pharmacokinetics

Abstract

The aim of this study was to evaluate the radiochemical behavior, biological distribution, and localization in infection sites in mice of a human polyclonal immunoglobulin (HIG) labelled with 99mTc by a novel MAG3-labelling method. The resulting [99mTc]MAG3-HIG was compared with [99mTc]HIG preparations radiolabelled directly via 2-mercaptoethanol (2-Me) or stannous ion (Sn) reduction and indirectly via 2-iminothiolane (2-Im) conjugation. All preparations showed similar UV and radioactivity HPLC profile to that of native HIG except for 2-Im-HIG, which showed aggregates. The stabilities of the label to challenge with cysteine were similar for all the preparations. By nondenaturing SDS-PAGE, all preparations other than MAG3-HIG showed evidence of lower molecular weight fragments. The tissue distribution 4 and 24 h after intravenous administration of the four preparations were compared in mice previously administered with an isolate of Staphylococcus aureus in one thigh. The pharmacokinetics varied among the different preparations. When prepared via 2-Me, Sn, and 2-Im, both blood clearance and urinary excretion were faster than that of labelled MAG3-HIG. The absolute uptake in the infected thigh at 24 h was significantly higher for HIG labelled via MAG3 and 2-Me vs. the remaining methods. The infected thigh/normal thigh radioactivity ratios were similar at both time points for labelled HIG prepared via 2-Me, 2-Im, and NHS-MAG, methods but was significantly lower at 24 h for HIG prepared via Sn. The radioactive HPLC profiles of serum at 4 and 24 h were similar to that of the radiolabelled injectates. Based on these data we conclude that each radiolabelled HIG preparation studied showed increased localization in infectious foci although [99Tc]MAG3-HIG showed superior radiochemical and biological characteristics under the conditions of this investigation.

Published

1998