Antithrombin-mediated Anticoagulant Activity of Sulfated Polysaccharides

Melo, Fabio Rabelo; Pereira, M. S.; Foguel, Débora; Mourāo, Paulo A.S.

doi:10.1074/jbc.m308688200

Cited by 146 publications

(116 citation statements)

References 46 publications

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“…With the examples described throughout the text, it is clear that the template mechanisms between SP (SF, SG, GAG), serpins (AT, HC-II) and protease (IIa) have differential stabilities or formation kinetics that are directly related to the structural features of the SP. and fully supports the expected bridging mechanism for the activity of SG, as previously described (Melo et al, 2004). Thus, both compounds are capable of interacting with AT, as indicated by theoretical results and experimental data showing that both polysaccharides are retained on an AT-affinity column.…”

Section: Preferential Conformation Binding-dependent Casesupporting

confidence: 59%

“…Anticoagulant activities of MSPs measured by APTT a and by IC50 for thrombin (IIa) and factor Xa inhibition in the presence of antithrombin (AT) or Heparin Cofactor II (HCII) (Pavão et al, 1998;Mourão, 2004;Pereira et al, 2005;Fonseca et al, 2008 Pavão et al, 1998. complex between heparin-AT-IIa ( Figure 4A), which supports the potentiation of this protease inactivation by AT in the presence of SG. This is an example of how the orientational constraints in solution can influence spatial preferences of the SP for their different bindings with target proteins (Melo et al, 2004). It is obvious that the difference in the sugar type drastically changes the conformation of the polymer as well, implying a different conformational binding, as explained in this section.…”

Section: Preferential Conformation Binding-dependent Casementioning

confidence: 99%

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Structure versus anticoagulant and antithrombotic actions of marine sulfated polysaccharides

Pomin¹,

Mourão²

2012

Rev. bras. farmacogn.

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Marine sulfated polysaccharides (MSP), such as sulfated fucans (SF), sulfated galactans (SG) and glycosaminoglycans (GAG) isolated from either algae or invertebrate animals, are highly anionic polysaccharides capable of interacting with certain cationic proteins, such as (co)-factors of the coagulation cascade during clotting-inhibition processes. These molecular complexes between MSP and coagulation-related proteins might, at first glance, be assumed to be driven mostly by electrostatic interactions. However, a systematic comparison using several novel sulfated polysaccharides composed of repetitive oligosaccharides with clear sulfation patterns has shown that these molecular interactions are regulated essentially by the stereochemistry of the glycans (which depends on a conjunction of anomericity, monosaccharide, conformational preference, and glycosylation and sulfation sites), rather than just a simple consequence of their negative charge density (mainly the number of sulfate groups). Here, we present an overview of the structure-function relationships of MSP, correlating their structures with their potential anticoagulant and antithrombotic actions, since pathologies related to the cardiovascular system are one of the major causes of illness and mortality in the world.

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Section: Preferential Conformation Binding-dependent Casesupporting

confidence: 59%

Section: Preferential Conformation Binding-dependent Casementioning

confidence: 99%

Structure versus anticoagulant and antithrombotic actions of marine sulfated polysaccharides

Pomin¹,

Mourão²

2012

Rev. bras. farmacogn.

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“…The results of anticoagulant activity indicated that the increasing of sulfate content from 15.04 % for UR to 25.68 % for URS resulting in an increasing of bioactivity. Melo et al [13] reported that the introduction of sulfate to polysaccharides increases the amount of negative charge. Then, the negatively charged sulfate groups can be combined with the positively charged groups from the coagulation protease inhibitor antithrombin, which can activate antithrombin and produce anticoagulant activity.…”

Section: Resultsmentioning

confidence: 99%

“…The results of 1 H và 13 C-NMR analysis were summarized in Table 1. The presence of sulfate groups after sulfation process was confirmed by FTIR and NMR spectra.…”

Section: Resultsmentioning

confidence: 99%

Effect of Sulfation on the Structure and Anticoagulant Activity of Ulvan Extracted From Green Seaweed Ulva Reticulata

Thu

2018

JST

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Ulvans are sulfated polysaccharides derived from the cell wall of green seaweeds. The chemical structure of ulvan extracted from Ulva reticulata is reported, focusing on investigation of the sulfated modification of the ulvan and the changes in structure and anticoagulant activity. The results showed that sulfated modification was able to change the ulvan conformational structure and markedly enhance its anticoagulant activity.

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“…Furthermore, the incidence of prion-related diseases in cows means that bovine heparin runs a risk of contamination which has to be carefully monitored. In the meantime, the ever-increasing demand for antithrombotic therapy calls for alternative sources of anticoagulant and antithrombotic compounds [8]. It has been shown that sulfated polysaccharides with anticoagulant activity are most abundant in marine invertebrates and marine algae [9,10].…”

Section: Preparation and Characterization Of Abalone Gonad Polysacchamentioning

confidence: 99%

Anticoagulant Activity and Structural Characterization of Polysaccharide from Abalone (Haliotis discus hannai Ino) Gonad

et al. 2016

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Abstract:In this study, we aimed at characterizing the structure and the anticoagulant activity of a polysaccharide fraction (AGP33) isolated from the gonads of Haliotis discus hannai Ino. AGP33 was extracted by enzymatic hydrolysis and purified by ion-exchange and gel-filtration chromatography. The backbone fraction of AGP33 (BAGP33), which appeared to contain of mannose, glucose and galactose, was prepared by partial acid hydrolysis. According to methylation and nuclear magnetic resonance (NMR) spectroscopy, the backbone of AGP33 was identified as mainly consisting of 1Ñ3-linked, 1Ñ4-linked, and 1Ñ6-linked monosaccharides. AGP33 is a sulfated polysaccharide with sulfates occur at 3-O-and 4-O-positions. It prolonged thromboplastin time (APTT), thrombin time (TT) and prothrombin time (PT) compared to a saline control solution in a dosage-dependent manner. AGP33 exhibited an extension (p < 0.01) of APTT compared to the saline group at concentrations higher than 5 µg/mL. AGP33 exhibited higher anticoagulant activity than its desulfated product (AGP33-des) and BAGP33. The results showed that polysaccharide with higher molecular weight and sulfate content demonstrated greater anticoagulant activity.

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Antithrombin-mediated Anticoagulant Activity of Sulfated Polysaccharides

Cited by 146 publications

References 46 publications

Structure versus anticoagulant and antithrombotic actions of marine sulfated polysaccharides

Structure versus anticoagulant and antithrombotic actions of marine sulfated polysaccharides

Effect of Sulfation on the Structure and Anticoagulant Activity of Ulvan Extracted From Green Seaweed Ulva Reticulata

Anticoagulant Activity and Structural Characterization of Polysaccharide from Abalone (Haliotis discus hannai Ino) Gonad

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