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Structural characterization and anti-inflammatory activity of two novel polysaccharides from the sea squirt, Ascidiella aspersa - 25/09/16

Doi : 10.1016/j.pupt.2016.05.001 
Derek Thomson b, Charalampos G. Panagos c, Radhakrishnan Venkatasamy a, Claire Moss b, Joanne Robinson b, Charles D. Bavington b, 1, John Hogwood a, d, Barbara Mulloy a, Dušan Uhrín c, Domenico Spina a, 1, Clive P. Page a, , 1
a Sackler Institute of Pulmonary Pharmacology, Institute of Pharmaceutical Science, King’s College London, SE1 9NH, UK 
b GlycoMar Ltd, European Centre for Marine Biotechnology, Oban, Scotland PA37 1QA, UK 
c EaStCHEM School of Chemistry, Joseph Black Building, The King’s Buildings, Edinburgh EH9 3JJ, UK 
d National Institute for Biological Standards and Control, South Mimms, Herts EN6 3QG, UK 

Corresponding author.

Abstract

It is now recognized that certain polysaccharides can exhibit anti-inflammatory activity, including the glycosaminoglycan (GAG) heparin that is widely used as an anti-coagulant drug. However, it would be desirable to identify molecules that retain the anti-inflammatory actions of heparin, but that are devoid of significant anti-coagulant activity. In the present study we have identified a number of novel GAG and GAG-like polysaccharides (VRP327) from marine organisms, most of which were resistant to digestion by heparinase II and chondroitinase ABC. Fourier transform infra-red spectrum (FTIR) revealed species with variable degrees of sulphation and monosaccharide analysis revealed a range of sugar compounds, which in some cases included sugars not present in mammalian GAGs. 1H NMR spectra of these species are consistent with the structures of complex polysaccharides. From an initial screening cascade to remove compounds having significant anti-coagulant activity and no overt cytotoxicity, we identified a high molecular weight oversulphated dermatan sulphate (VRP327) isolated from the tunicate Ascidiella aspersa which was fully characterised by NMR spectroscopy. This material was depolymerised to produce well characterized low molecular weight fractions which were demonstrated to be non-toxic, with low levels of anti-coagulant activity, and to have demonstrable anti-inflammatory activity assessed in several in vitro and in vivo models. The identification of low molecular weight polysaccharides having significant anti-inflammatory activity without significant anti-coagulant activity may provide novel templates for the development of a novel class of anti-inflammatory drugs.

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Keywords : Glycosaminoglycans, Adhesion, Elastase, Inflammation, Marine organisms


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Vol 40

P. 69-79 - octobre 2016 Retour au numéro
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