Your search keyword '"Erika Marzola"' showing total 2 results

1. Design and Synthesis of 99mTcN-Labeled Dextran-Mannose Derivatives for Sentinel Lymph Node Detection

Author

Alessandra Boschi, Micòl Pasquali, Claudio Trapella, Alessandro Massi, Petra Martini, Adriano Duatti, Remo Guerrini, Vinicio Zanirato, Anna Fantinati, Erika Marzola, Melchiore Giganti, and Licia Uccelli

Subjects

sentinel lymph node, dextran, mannose, 99mTc-radiopharmaceuticals, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Background: New approaches based on the receptor-targeted molecular interaction have been recently developed with the aim to investigate specific probes for sentinel lymph nodes. In particular, the mannose receptors expressed by lymph node macrophages became an attractive target and different multifunctional mannose derivate ligands for the labeling with 99mTc have been developed. In this study, we report the synthesis of a specific class of dextran-based, macromolecular, multifunctional ligands specially designed for labeling with the highly stable [99mTc≡N]2+ core. Methods: The ligands have been obtained by appending to a macromolecular dextran scaffold pendant arms bearing a chelating moiety for the metallic group and a mannosyl residue for allowing the interaction of the resulting macromolecular 99mTc conjugate with specific receptors on the external membrane of macrophages. Two different chelating systems have been selected, S-methyl dithiocarbazate [H2N‒NH‒C(=S)SCH3=HDTCZ] and a sequence of two cysteine residues, that in combination with a monophosphine coligand, are able to bind the [99mTc≡N]2+ core. Conclusions: High-specific-activity labeling has been obtained by simple mixing and heating of the [99mTc≡N]2+ group with the new mannose-dextran derivatives.

Published

2018

2. Design and Synthesis of 99mTcN-Labeled Dextran-Mannose Derivatives for Sentinel Lymph Node Detection

Author

Claudio Trapella, Remo Guerrini, Anna Fantinati, Micol Pasquali, Petra Martini, Melchiore Giganti, Licia Uccelli, Alessandro Massi, Alessandra Boschi, Erika Marzola, Adriano Duatti, and Vinicio Zanirato

Subjects

Stereochemistry, 99mTc-radiopharmaceuticals, lcsh:Medicine, lcsh:RS1-441, Pharmaceutical Science, Mannose, Article, 030218 nuclear medicine & medical imaging, NO, lcsh:Pharmacy and materia medica, 03 medical and health sciences, chemistry.chemical_compound, Residue (chemistry), 0302 clinical medicine, sentinel lymph node, Drug Discovery, Moiety, Chelation, Dextran, Sentinel lymph node, Molecular Medicine, 3003, mannose, lcsh:R, chemistry, 030220 oncology & carcinogenesis, dextran, Macromolecule, Cysteine, Conjugate

Abstract

Background: New approaches based on the receptor-targeted molecular interaction have been recently developed with the aim to investigate specific probes for sentinel lymph nodes. In particular, the mannose receptors expressed by lymph node macrophages became an attractive target and different multifunctional mannose derivate ligands for the labeling with 99mTc have been developed. In this study, we report the synthesis of a specific class of dextran-based, macromolecular, multifunctional ligands specially designed for labeling with the highly stable [99mTc&equiv, N]2+ core. Methods: The ligands have been obtained by appending to a macromolecular dextran scaffold pendant arms bearing a chelating moiety for the metallic group and a mannosyl residue for allowing the interaction of the resulting macromolecular 99mTc conjugate with specific receptors on the external membrane of macrophages. Two different chelating systems have been selected, S-methyl dithiocarbazate [H2N‒NH‒C(=S)SCH3=HDTCZ] and a sequence of two cysteine residues, that in combination with a monophosphine coligand, are able to bind the [99mTc&equiv, N]2+ core. Conclusions: High-specific-activity labeling has been obtained by simple mixing and heating of the [99mTc&equiv, N]2+ group with the new mannose-dextran derivatives.

Published

2018