Importance of a 3-O-sulfate Group in a Heparin Pentasaccharide for Antithrombotic Activity
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Previous theoretical and experimental evidence led to the formulation of a specific pentasaccharide structure which represents the site in heparin for binding to antithrombin III. This pentasaccharide was subsequently synthesized. A pentasaccharide of the same structure but lacking only the sulfate group on the hydroxyl group of the middle glucosamine (position C-3) was also synthesized to test the structure - activity relationships. Previous biochemical studies showed the 3-O-desulfated pentasaccharide to have a low affinity binding to AT III and to be devoid of the high anti-factor Xa activity characteristic of the pentasaccharide. Our in vivo studies, in a venous stasis thrombosis model proved the 3-O-desulfated pentasaccharide, at equigravimetric dosages, to be devoid of the antithrombotic activity previously reported for the pentasaccharide. These studies confirm the fact that inhibition of factor Xa at a high level of activity produces an antithrombotic effect.
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Zhao W, Garron M, Yang B, Xiao Z, Esko J, Cygler M FEBS Lett. 2011; 585(15):2461-6.
PMID: 21741976 PMC: 3338322. DOI: 10.1016/j.febslet.2011.06.023.
Park S, Jiang R, Piao S, Zhang B, Kim E, Kwon H J Biol Chem. 2010; 286(2):1567-75.
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Johnson D, Langdown J, Huntington J Proc Natl Acad Sci U S A. 2010; 107(2):645-50.
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