(TC)-T-99m-N-IFC: a new isoniazid derivative for Mycobacterium diagnostic
| Autor: | Essouissi, I., Saied, N. Malek, Bernardin, Serge, Guizani, S., Mejri, N., LEROUX-BARC, Celine, Ben Hamouda, S., Asmi, A., Saïdi, M. |
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| Přispěvatelé: | Unit Med Agr & Environm Tech Nucl Applicat CNSTN, Partenaires INRAE, Plateforme d'Infectiologie Expérimentale (PFIE), Institut National de la Recherche Agronomique (INRA) |
| Jazyk: | angličtina |
| Rok vydání: | 2012 |
| Předmět: | |
| Zdroj: | Radiochimica Acta Radiochimica Acta, Oldenbourg Wissenschaftsverlag, 2012, 100 (3), pp.207-214. ⟨10.1524/ract.2012.1905⟩ |
| ISSN: | 0033-8230 2193-3405 |
| DOI: | 10.1524/ract.2012.1905⟩ |
| Popis: | International audience; We present in this work a new technetium-99m-labeled derivative from isoniazid. The labeling was achieved with a double-ligand transfer through the use of a ferrocene derivative. A further referred to as Tc-99m-N-IFC (N-Isonicotinamide ferrocene carboxamide labeled with Tc-99m), targeting infections in experimental animals, has been synthesized. The N-IFC was chemically synthesized and then labeled with technetium-99m. It has been confirmed through this work that it was obtained with high radiolabelling yield (95%). Radiochemical analyses of Tc-99m-N-IFC revealed that the molecule was efficiently labeled with a little free pertechnetate in the preparations containing purified compound. Only 1-2% of the tracer was leached out from the complex at 24 h when incubated in serum at 37 degrees C confirmed its high stability. The radiolabeled complex was found to be 10% bound to blood protein, which corresponds to a fast retention advantage. Biodistribution study showed the renal route of excretion and has also demonstrated that our radiolabeled compound is rapidly and significantly accumulated (P < 0.5) at infection sites. Thigh model of localized infection was prepared in mice by injecting of BCG (pGFM-11) (fluorexcente BCG) live bacteria in growing phase. The confirmation of the bacteria presence in infection sites has been established through its fluorescence characteristic. The comparison of the Tc-99m-N-IFC accumulation at sites of BCG (pGFM-11) infected animals, which is expressed as target-to-non-target ratio, (3.14) with other radiotracers was discussed. This allowed us to consider that Tc-99m-N-IFC could be a good radiotracer for mycobacterial infections. Obtained results were in good and encourage to undergo a similar labeling for the Mycobacterium tuberculosis as perspective of this work. |
| Databáze: | OpenAIRE |
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