Synthesis of thrombin-inhibiting heparin mimetics without side effects

Petitou, Maurice; Hérault, Jean-Pascal; Bernat, A; Driguez, Pierre‐Alexandre; Duchaussoy, Philippe; Lormeau, J C; Herbert, Jean‐Marc

doi:10.1038/18877

Cited by 317 publications

(235 citation statements)

References 26 publications

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“…A comprehensive study of the relationship of the saccharide sequences and gDbinding affinity remains to be investigated when a series of structurally defined HS oligosaccharides are available. The structural information from this study will serve as a lead compound for the chemical synthesis of HS oligosaccharides for further investigation (45).…”

Section: Discussionmentioning

confidence: 99%

Characterization of a Heparan Sulfate Octasaccharide That Binds to Herpes Simplex Virus Type 1 Glycoprotein D

Liu

Shriver

Pope

et al. 2002

Journal of Biological Chemistry

153

116

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Herpes simplex virus type 1 utilizes cell surface heparan sulfate as receptors to infect target cells. The unique heparan sulfate saccharide sequence offers the binding site for viral envelope proteins and plays critical roles in assisting viral infections. A specific 3-O-sulfated heparan sulfate is known to facilitate the entry of herpes simplex virus 1 into cells. The 3-O-sulfated heparan sulfate is generated by the heparan sulfate D-glucosaminyl-3-O-sulfotransferase isoform 3 (3-OST-3), and it provides binding sites for viral glycoprotein D (gD). Here, we report the purification and structural characterization of an oligosaccharide that binds to gD. The isolated gDbinding site is an octasaccharide, and has a binding affinity to gD around 18 M, as determined by affinity coelectrophoresis. The octasaccharide was prepared and purified from a heparan sulfate oligosaccharide library that was modified by purified 3-OST-3 enzyme. The molecular mass of the isolated octasaccharide was determined using both nanoelectrospray ionization mass spectrometry and matrix-assisted laser desorption/ionization mass spectrometry. The results from the sequence analysis suggest that the structure of the octasaccharide is a heptasulfated octasaccharide. The proposed structure of the octasaccharide is ⌬UA-GlcNSIdoUA2S-GlcNAc-UA2S-GlcNS-IdoUA2S-GlcNH 2 3S6S. Given that the binding of 3-O-sulfated heparan sulfate to gD can mediate viral entry, our results provide structural information about heparan sulfate-assisted viral entry.Heparan sulfates (HS), 1 highly sulfated polysaccharides, are present on the surface of mammalian cells and in the extracellular matrix in large quantities. HS play critical roles in a variety of biological interactions, including assisting viral infection, regulating blood coagulation and embryonic development, suppressing tumor growth, and controlling the eating behavior of mice by interacting with specific regulatory proteins (1-5). HS is initially synthesized as a copolymer of glucuronic acid and N-acetylated glucosamine by D-glucuronyl and N-acetyl-D-glucosaminyl transferase, followed by various modifications (6). These modifications include C 5 -epimerization of glucuronic acid to form iduronic acid residues, 2-O-sulfation of iduronic and glucuronic acid, N-deacetylation and N-sulfation of glucosamine, as well as 6-O-sulfation and 3-O-sulfation of glucosamine. Numerous HS biosynthetic enzymes have been cloned and characterized (for review, see Esko and Lindahl (7)).The specific sulfated saccharide sequences play critical roles in determining the functions of HS. A recent report suggests that the expression levels of various isoforms of each class of HS biosynthetic enzyme contribute to the synthesis of specific saccharide sequences in specific tissues (8). HS N-deacetylase/ N-sulfotransferase, 3-O-sulfotransferase, and 6-O-sulfotransferase are present in multiple isoforms, and each isoform is believed to recognize the saccharide sequence around the modification site to generate a specific sulfated saccharid...

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Section: Discussionmentioning

confidence: 99%

Characterization of a Heparan Sulfate Octasaccharide That Binds to Herpes Simplex Virus Type 1 Glycoprotein D

Liu

Shriver

Pope

et al. 2002

Journal of Biological Chemistry

153

116

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“…Heparins-Synthetic pentasaccharide and hexadecasaccharide heparins containing the antithrombin binding sequence (5,37) were provided by Maurice Petitou of Sanofi-Aventis Recherche (Toulouse, France). A full-length heparin containing the pentasaccharide binding sequence and ϳ50 saccharides in length was isolated from commercial heparin by size and affinity fractionation as described previously (30).…”

Section: Methodsmentioning

confidence: 99%

“…Reaction with factor Xa Binding of S195A Factor Xa to the Labeled AntithrombinsThe ϳ40% fluorescence increase accompanying the addition of S195A factor Xa to P7-NBD-antithrombin-heparin complex allowed quantitation of the binding affinity of the inactive factor Xa for antithrombin in the absence and presence of the heparin pentasaccharide and a hexadecasaccharide heparin mimetic capable of bridging antithrombin and proteases (37). Titrations of S195A factor Xa into P7-NBD-antithrombin complexed with the natural pentasaccharide, a higher affinity pentasaccharide, (5) or the hexadecasaccharide heparin resulted in saturable increases in fluorescence of comparable magnitude ( Fig.…”

Section: Reaction With Thrombinmentioning

confidence: 99%

Mechanism by Which Exosites Promote the Inhibition of Blood Coagulation Proteases by Heparin-activated Antithrombin

Izaguirre

Swanson

Raja

et al. 2007

Journal of Biological Chemistry

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Heparin activates the serpin, antithrombin, to inhibit its target blood-clotting proteases by generating new protease interaction exosites. To resolve the effects of these exosites on the initial Michaelis docking step and the subsequent acylation and conformational change steps of antithrombin-protease reactions, we compared the reactions of catalytically inactive S195A and active proteases with site-specific fluorophore-labeled antithrombins that allow monitoring of these reaction steps. Heparin bound to N,N-dimethyl-N-(acetyl)-N-(7-nitrobenz-3-oxa-1,3-diazol-4-yl)ethylenediamine (NBD)-fluorophore-labeled antithrombins and accelerated the reactions of the labeled inhibitor with thrombin and factor Xa similar to wild type. Equilibrium binding of NBD-labeled antithrombins to S195A proteases showed that exosites generated by conformationally activating antithrombin with a heparin pentasaccharide enhanced the affinity of the serpin for S195A factor Xa minimally 100-fold. Moreover, additional bridging exosites provided by a hexadecasaccharide heparin activator enhanced antithrombin affinity for both S195A factor Xa and thrombin at least 1000-fold. Rapid kinetic studies showed that these exosite-mediated enhancements in Michaelis complex affinity resulted from increases in k on and decreases in k off and caused antithrombin-protease reactions to become diffusion-controlled. Competitive binding and kinetic studies with exosite mutant antithrombins showed that Tyr-253 was a critical mediator of exosite interactions with S195A factor Xa; that Glu-255, Glu-237, and Arg-399 made more modest contributions to these interactions; and that exosite interactions reduced k off for the Michaelis complex interaction. Together these results show that exosites generated by heparin activation of antithrombin function both to promote the formation of an initial antithrombin-protease Michaelis complex and to favor the subsequent acylation of this complex.

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“…The structural requirement for binding of this oligosaccharide to thrombin, a cluster of sulfated saccharide units, appears to be less selective than for AT. Petitou and colleagues proved that the order of the three domains is essential for thrombin inhibition (19). Namely, the ATbinding domain is positioned at the reducing end of the nonsulfated linker, and the thrombinbinding domain at the nonreducing end of the linker.…”

Section: Structure and Anticoagulant Activity Relationshipmentioning

confidence: 99%

“…However, the pentasaccharide unit only inhibits the activity of factor Xa mediated by AT. A much larger oligosaccharide is required to exhibit complete anti-thrombin activity (18,19). Selectivity for HS by protein binding partners stems from a number of different structural variables that affect the overall charge and conformation.…”

Section: Structure and Anticoagulant Activity Relationshipmentioning

confidence: 99%

Anticoagulant heparan sulfate: structural specificity and biosynthesis

Liu

Pedersen

2007

Appl Microbiol Biotechnol

123

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SummaryHeparan sulfate (HS) is present on the surface of endothelial and surrounding tissues in large quantities. It plays important roles in regulating numerous functions of the blood vessel wall, including blood coagulation, inflammation response and cell differentiation. HS is a highly sulfated polysaccharide containing glucosamine and glucuronic/iduronic acid repeating disaccharide units. The unique sulfated saccharide sequences of HS determine its specific functions. Heparin, an analogue of heparan sulfate, is the most commonly used anticoagulant drug. Because of its wide range of biological functions, HS has become an interesting molecule to biochemists, medicinal chemists and developmental biologists. Here, we summarize recent progress towards understanding the interaction between heparan sulfate and blood coagulating factors, the biosynthesis of anticoagulant heparan sulfate and the mechanism of action of heparan sulfate biosynthetic enzymes. Further, knowledge of the biosynthesis of HS facilitates the development of novel enzymatic approaches to synthesize HS from bacterial capsular polysaccharides and to produce polysaccharide end products with high specificity for the biological target. These advancements provide the foundation for the development of polysaccharide-based therapeutic agents.

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Synthesis of thrombin-inhibiting heparin mimetics without side effects

Cited by 317 publications

References 26 publications

Characterization of a Heparan Sulfate Octasaccharide That Binds to Herpes Simplex Virus Type 1 Glycoprotein D

Characterization of a Heparan Sulfate Octasaccharide That Binds to Herpes Simplex Virus Type 1 Glycoprotein D

Mechanism by Which Exosites Promote the Inhibition of Blood Coagulation Proteases by Heparin-activated Antithrombin

Anticoagulant heparan sulfate: structural specificity and biosynthesis

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