Doubly radiolabeled liposomes for pretargeted radioimmunotherapy
Autor: | Marie Mougin-Degraef, Catherine Saï-Maurel, Mickaël Bourgeois, Philippe Thedrez, Alain Faivre-Chauvet, Jacques Barbet, C. Bourdeau, Emmanuelle Jestin, Jean-François Gestin, P. Remaud-Le Saec |
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Rok vydání: | 2007 |
Předmět: |
Biodistribution
medicine.medical_treatment Succinimides Pharmaceutical Science Arginine Iodine Radioisotopes Mice Drug Delivery Systems Drug Stability Pharmacokinetics In vivo medicine Animals Tissue Distribution Pretargeted Radioimmunotherapy Mice Inbred BALB C Liposome Chromatography Chemistry Vesicle Indium Radioisotopes Radioimmunotherapy Isotope Labeling Liposomes Female Indicators and Reagents Conjugate |
Zdroj: | International Journal of Pharmaceutics. 344:110-117 |
ISSN: | 0378-5173 |
Popis: | The aim of this study was to design liposomes as radioactivity carriers for pretargeted radioimmunotherapy with favorable pharmacokinetic parameters. To monitor the liposomes integrity in vivo, their surface was radiolabeled with indium-111 bound to DTPA-derivatized phosphatidylethanolamine (DSPE-DTPA) and the aqueous phase was labeled by using an original active loading technique of radioiodinated Bolton-Hunter reagent (BH) that reacts with pre-encapsulated arginine to form a positively charged conjugate ((125)I-BH-arginine). Different formulations of doubly radiolabeled liposomes were tested in vitro and in vivo to evaluate radiolabeling stability, integrity of the vesicles and their pharmacokinetics. Radiolabeling yields were high (surface >75%, encapsulation >60%) and stable (>85% after 24 h in serum 37 degrees C). In vivo, the pharmacokinetic behavior of doubly radiolabeled liposomes was strongly dependant on the formulation. Blood clearance of PEGylated liposomes (DSPC/Chol/DSPE-DTPA/DSPE-PEG5%) was 0.15 mL/h compared to a conventional formulation (DSPC/Chol/DSPE-DTPA: clearance 1.44 mL/h). Non-encapsulated BH-arginine conjugate was quickly eliminated in urine (clearance 6.04 mL/h). Blood kinetics of the two radionuclides were similar and radiochromatographic profiles of mice serum confirmed the integrity of circulating liposomes. The significant reduction of activity uptake in organs after liposome catabolism (liver and spleen), achieved by the rapid renal elimination of (125)I-BH-arginine, should bring significant improvements for targeted radionuclide therapy with sterically-stabilized liposomes. |
Databáze: | OpenAIRE |
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