A novel procedure for the high-yield preparation of Re-188 radiopharmaceuticals containing a terminal ReN multiple bond is described. This method involves the reaction of [188Re][ReO4] with N-methyl S-methyl dithiocarbazate (DTCZ), as donor of nitrido nitrogen atoms, sodium oxalate and SnCl2 to afford a mixture of two intermediate compounds. When this mixture is reacted with the sodium salt of a dithiocarbamate ligand (L) of the type Na[R2N-C(S)S] (R CH3, CH3CH2, CH3CH2CH2), the formation of the bis-substituted, neutral complexes [188Re][Re(N)(L)2] is easily obtained in high yield ( 95%). The complexes [188Re][Re(N)(L)2] were characterized by chromatographic methods, and by comparison with the corresponding complexes prepared at macroscopic level starting from a nonradioactive rhenium precursor. Biodistribution studies were carried out in rats. Results showed that the complexes [188Re][Re(N)(L)2] exhibited the same biological behavior of the analogous Tc-99m complexes reported previously. The easy application of the new synthetic procedure indicates that it could be conveniently employed for preparing a large class of new Re-188 complexes having potential utilization in nuclear medicine as therapeutic agents. © 2003 Elsevier Inc. All rights reserved.

High-yield synthesis of the terminal Re-188 N multiple bond from generator-produced [(ReO4)-Re-188](-)

BOSCHI, Alessandra;UCCELLI, Licia;DUATTI, Adriano
2003

Abstract

A novel procedure for the high-yield preparation of Re-188 radiopharmaceuticals containing a terminal ReN multiple bond is described. This method involves the reaction of [188Re][ReO4] with N-methyl S-methyl dithiocarbazate (DTCZ), as donor of nitrido nitrogen atoms, sodium oxalate and SnCl2 to afford a mixture of two intermediate compounds. When this mixture is reacted with the sodium salt of a dithiocarbamate ligand (L) of the type Na[R2N-C(S)S] (R CH3, CH3CH2, CH3CH2CH2), the formation of the bis-substituted, neutral complexes [188Re][Re(N)(L)2] is easily obtained in high yield ( 95%). The complexes [188Re][Re(N)(L)2] were characterized by chromatographic methods, and by comparison with the corresponding complexes prepared at macroscopic level starting from a nonradioactive rhenium precursor. Biodistribution studies were carried out in rats. Results showed that the complexes [188Re][Re(N)(L)2] exhibited the same biological behavior of the analogous Tc-99m complexes reported previously. The easy application of the new synthetic procedure indicates that it could be conveniently employed for preparing a large class of new Re-188 complexes having potential utilization in nuclear medicine as therapeutic agents. © 2003 Elsevier Inc. All rights reserved.
2003
Boschi, Alessandra; C., Bolzati; Uccelli, Licia; Duatti, Adriano
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11392/1201636
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