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  4. Improved antithrombotic activity and diminished bleeding side effect of a PEGylated alphaiIb beta 3 antagonist, disintegrin
 
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Improved antithrombotic activity and diminished bleeding side effect of a PEGylated alphaiIb beta 3 antagonist, disintegrin

Journal
Thrombosis Research
Journal Volume
143
Pages
3-10
Date Issued
2016
Author(s)
Hsu C.-C.
Chuang W.-J.
Chung C.-H.
Chang C.-H.
Peng H.-C.
TUR-FU HUANG  
DOI
10.1016/j.thromres.2016.04.020
URI
https://scholars.lib.ntu.edu.tw/handle/123456789/564111
Abstract
Introduction The applicability of protein drugs is confined by protein degradation and rapid elimination. PEGylation of polypeptides improves protein stability by sterically obstructing the degradation by serum proteases and reduces renal clearance by the increased mass. Experimental approach We compared the antithrombotic activities of intact rhodostomin (Rn) and PEGylated rhodostomin (PRn) both in vitro and in vivo systems. In addition, the functional half-life in inhibiting platelet aggregation and the tendency in causing bleeding side effect were investigated. Results Rn and PRn both potently inhibited human and mouse platelet aggregation induced by collagen, thrombin or ADP in vitro with a similar IC50 around 60-100 nM. Rotational thromboelastometry assay indicated that PRn was more effective than Rn in preventing clot formation in human whole blood. In platelet-rich plasma from mice injected with Rn or PRn, the inhibitory effects on collagen-induced platelet aggregation were also comparable, but Rn caused higher bleeding tendency. In ferric chloride-induced arterial thrombosis, Rn and PRn significantly prolonged occlusion time at high dosage (0.2 μg/g). However, PRn obviously prolonged the occlusion time even given at a lower dosage (0.06 μg/g). The functional half-life assay revealed that PEGylation prolonged the in vivo half-life of Rn. Conclusions PRn exhibits higher antithrombotic potency and longer half-life in vivo as compared with native Rn on a molar basis. In addition, PRn exhibits a better safety profile at an efficacious antithrombotic dose in vivo. Therefore, PEGylation may be one of the ideal options in modifying disintegrin derivatives as the safe therapeutic agents for integrin-related diseases. ? 2016 Published by Elsevier Ltd.
SDGs

[SDGs]SDG3

Other Subjects
adenosine diphosphate; anticoagulant agent; disintegrin; rhodostomin; thrombin; unclassified drug; antithrombocytic agent; disintegrin; fibrinogen receptor; macrogol derivative; peptide; rhodostomin; animal experiment; animal tissue; anticoagulation; artery thrombosis; Article; bleeding; blood sampling; controlled study; drug half life; drug safety; human; IC50; in vitro study; in vivo study; male; mouse; nonhuman; polyacrylamide gel electrophoresis; priority journal; thrombocyte aggregation; thrombocyte aggregation inhibition; thrombocyte count; thrombocyte rich plasma; thromboelastography; Western blotting; animal; antagonists and inhibitors; bleeding; blood; chemically induced; chemistry; drug effects; drug stability; half life time; Institute for Cancer Research mouse; metabolism; protein stability; thrombocyte; thrombosis; Animals; Blood Platelets; Disintegrins; Drug Stability; Half-Life; Hemorrhage; Humans; Male; Mice; Mice, Inbred ICR; Peptides; Platelet Aggregation; Platelet Aggregation Inhibitors; Platelet Glycoprotein GPIIb-IIIa Complex; Polyethylene Glycols; Protein Stability; Thrombosis
Type
journal article

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