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来自哈氏仙掌藻的硫酸化木聚糖的抗疱疹活性。

Anti-herpetic activity of a sulfated xylomannan from Scinaia hatei.

作者信息

Mandal Pinaki, Pujol Carlos A, Carlucci María J, Chattopadhyay Kausik, Damonte Elsa B, Ray Bimalendu

机构信息

Natural Products Laboratory, Department of Chemistry, The University of Burdwan, Golapbag, Burdwan, West Bengal 713 104, India.

出版信息

Phytochemistry. 2008 Aug;69(11):2193-9. doi: 10.1016/j.phytochem.2008.05.004. Epub 2008 Jun 21.

Abstract

Many viruses display affinity for cell surface heparan sulfate proteoglycans with biological relevance in virus entry. This raises the possibility of the application of sulfated polysaccharides in antiviral therapy. In this study we have analyzed polysaccharide fractions isolated from Scinaia hatei. The crude water extract (ShWE) as well as one fraction (F1) obtained by size exclusion chromatography had potent anti-HSV activity. Their inhibitory concentration 50% (IC50) values ranging from 0.5 to 4.6 microg/ml were much lower than the cytotoxic concentration 50% (CC50) values (1000 microg/ml). These fractions had very low anticoagulant activity. Furthermore, they had a weak inactivating effect on virions in a virucidal assay at concentrations in the range of 60-100 microg/ml. Chemical, chromatographic and spectroscopic methods showed that the major polysaccharide, which had 0.4 sulfate group per monomer unit and an apparent molecular mass of 160 kDa, contained a backbone of alpha-(1-->3)-linked D-mannopyranosyl residues substituted at C-6, C-4 and C-2 with single stub of beta-d-xylopyranosyl residues. Sulfate groups, when present, are located at C-4 of alpha-(1-->3)-linked D-mannopyranosyl units, and appeared to be very important for the anti-herpetic activity of this polymer.

摘要

许多病毒对细胞表面硫酸乙酰肝素蛋白聚糖具有亲和力,这在病毒进入过程中具有生物学相关性。这增加了硫酸化多糖在抗病毒治疗中应用的可能性。在本研究中,我们分析了从哈氏仙菜中分离得到的多糖组分。粗水提取物(ShWE)以及通过尺寸排阻色谱法获得的一个组分(F1)具有强大的抗单纯疱疹病毒(HSV)活性。它们的半数抑制浓度(IC50)值在0.5至4.6微克/毫升之间,远低于半数细胞毒性浓度(CC50)值(1000微克/毫升)。这些组分具有非常低的抗凝活性。此外,在浓度为60 - 100微克/毫升的杀病毒试验中,它们对病毒粒子的灭活作用较弱。化学、色谱和光谱方法表明,主要多糖每个单体单元含有0.4个硫酸基团,表观分子量为160 kDa,其主链由α-(1→3)-连接的D-甘露吡喃糖基残基组成,在C-6、C-4和C-2位被单个β-D-木吡喃糖基残基取代。当存在硫酸基团时,它们位于α-(1→3)-连接的D-甘露吡喃糖基单元的C-4位,并且似乎对该聚合物的抗疱疹活性非常重要。

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