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Anti-HIV-1 activity of low molecular weight sulfated chitooligosaccharides

机译:低分子量硫酸化壳寡糖的抗HIV-1活性

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Chitooligosaccharides are nontoxic and water-soluble compounds obtained by enzymatic degradation of chitosan, which is derived from chitin by a deacetylation process. Chitooligosaccharides possess broad range of activities such as antitumour, antifungal, antibacterial activities. Sulfated chitooligosaccharides (SCOSs) with different molecular weights were synthesized by a random sulfation reaction. In the present study, anti-HIV-1 properties of SCOSs and the impact of molecular weight on their inhibitory activity were investigated. SCOS III (MW 3-5 kDa) was found to be the most effective compound to inhibit HIV-1 replication. At nontoxic concentrations, SCOS III exhibited remarkable inhibitory activities on HIV-1-induced syncytia formation (EC50 2.19 mu g/ml), lytic effect (EC50 1.43 mu g/ml), and p24 antigen production (EC50 4.33 mu g/ml and 7.76 mu g/ml for HIV-1(RF) and HIV-1(Ba-L), respectively). In contrast, unsulfated chitooligosaccharides showed no activity against HIV-1. Furthermore, it was found that SCOS III blocked viral entry and virus-cell fusion probably via disrupting the binding of HIV-1 gp120 to CD4 cell surface receptor. These results suggest that sulfated chitooligosaccharides represent novel candidates for the development of anti-HIV-1 agent.
机译:壳寡糖是通过壳聚糖的酶促降解而获得的无毒且水溶性的化合物,壳聚糖是通过脱乙酰过程从几丁质衍生而来的。壳寡糖具有广泛的活性,例如抗肿瘤,抗真菌,抗菌活性。通过随机硫酸化反应合成了不同分子量的硫酸化壳寡糖(SCOSs)。在本研究中,研究了SCOS的抗HIV-1特性以及分子量对其抑制活性的影响。发现SCOS III(MW 3-5 kDa)是抑制HIV-1复制的最有效化合物。在无毒浓度下,SCOS III对HIV-1诱导的合胞体形成(EC50 2.19μg / ml),溶解作用(EC50 1.43μg/ ml)和p24抗原产生(EC50 4.33μg/ ml和HIV-1(RF)和HIV-1(Ba-L)分别为7.76微克/毫升)。相反,未硫酸化的壳寡糖对HIV-1没有活性。此外,发现SCOS III可能通过破坏HIV-1 gp120与CD4细胞表面受体的结合来阻止病毒进入和病毒细胞融合。这些结果表明,硫酸化的壳寡糖代表了抗HIV-1剂开发​​的新候选者。

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