Pharmaceutical Development and Safety Evaluation of a GMP-Grade Fucoidan for Molecular Diagnosis of Cardiovascular Diseases

The adhesion molecule P-selectin is present on the cell surface of both activated endothelium and activated platelets. The present study describes the pharmaceutical development, safety evaluation, and preclinical efficacy of a micro-dosed radiotracer. The macromolecular nanoscale assembly consisted...

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Veröffentlicht in:Marine drugs 2019-12, Vol.17 (12), p.699
Hauptverfasser: Chauvierre, Cédric, Aid-Launais, Rachida, Aerts, Joël, Chaubet, Frédéric, Maire, Murielle, Chollet, Lucas, Rolland, Lydia, Bonafé, Roberta, Rossi, Silvia, Bussi, Simona, Cabella, Claudia, Dézsi, Laszlo, Fülöp, Tamas, Szebeni, Janos, Chahid, Youssef, Zheng, Kang H, Stroes, Erik S G, Le Guludec, Dominique, Rouzet, François, Letourneur, Didier
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Sprache:eng
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Zusammenfassung:The adhesion molecule P-selectin is present on the cell surface of both activated endothelium and activated platelets. The present study describes the pharmaceutical development, safety evaluation, and preclinical efficacy of a micro-dosed radiotracer. The macromolecular nanoscale assembly consisted of a natural compound made of a sulfated fucose-rich polysaccharides (fucoidan) and a radionuclide (technetium-99m) for the detection of -selectin expression in cardiovascular diseases. After extraction and fractionation from brown seaweeds, the good manufacturing practice (GMP) production of a low molecular weight (LMW) fucoidan of 7 kDa was achieved and full physicochemical characterization was performed. The regulatory toxicology study in rats of the GMP batch of LMW fucoidan revealed no adverse effects up to 400 μg/kg (×500 higher than the expected human dose) and pseudoallergy was not seen as well. In a myocardial ischemia-reperfusion model in rats, the GMP-grade LMW fucoidan labeled with technetium-99m detected -selectin upregulation in vivo. The present study supports the potential of using Tc-fucoidan as an imaging agent to detect activated endothelium in humans.
ISSN:1660-3397
1660-3397
DOI:10.3390/md17120699