Department of Biochemistry, School of Pharmaceutical Sciences, University of Shizuoka, and Global COE Program for Innovation in Human Health Sciences, 52-1 Yada, Suruga-ku, Shizuoka-shi, Shizuoka 422-8526, Japan.
Antiviral Res. 2010 Nov;88(2):236-43. doi: 10.1016/j.antiviral.2010.09.002. Epub 2010 Sep 21.
Sulphated glycosaminoglycans such as heparin inhibit the early step of dengue virus infection through interaction with envelope (E) protein. Here, we found that chondroitin sulphate E (CSE), but not CSD, which contains the same degree of sulphation, inhibited dengue virus (DENV) infection of cells with adsorption. CSE significantly reduced infectivity of all dengue virus serotypes to BHK-21 and Vero cells. DENV preferentially bound to CSE immobilised on plastic plates. Also, virus binding to CSE or heparin was cross-inhibited by soluble CSE or heparin. These findings suggested that common carbohydrate determinants on CSE and heparin could be essential epitopes for interaction of DENV, and may be responsible for inhibition of the early steps of DENV infection. A recombinant E protein directly bound heparin and CSE, but not CSD, meaning that interaction of CSE with E protein contributes to the inhibitory action of this glycosaminoglycan. These observations indicate that a specific carbohydrate structure rather than polysulphation or addition of negative charges of the glycosaminoglycan molecule would be necessary for direct binding to DENV E protein. In conclusion, CSE showed antiviral activity as an entry inhibitor targeting E protein of dengue virus.
硫酸化糖胺聚糖如肝素通过与包膜 (E) 蛋白相互作用抑制登革热病毒感染的早期步骤。在这里,我们发现硫酸软骨素 E (CSE),而不是含有相同硫酸化程度的硫酸软骨素 D (CSD),通过吸附抑制登革热病毒 (DENV) 感染细胞。CSE 显著降低了所有登革热病毒血清型对 BHK-21 和 Vero 细胞的感染性。DENV 优先与固定在塑料板上的 CSE 结合。此外,病毒与 CSE 或肝素的结合可被可溶性 CSE 或肝素交叉抑制。这些发现表明,CSE 和肝素上的共同碳水化合物决定簇可能是 DENV 相互作用的必需表位,可能是抑制 DENV 感染早期步骤的原因。重组 E 蛋白直接结合肝素和 CSE,但不结合 CSD,这意味着 CSE 与 E 蛋白的相互作用有助于该糖胺聚糖的抑制作用。这些观察结果表明,对于与 DENV E 蛋白的直接结合,糖胺聚糖分子的特定碳水化合物结构而不是多硫酸化或负电荷的增加是必要的。总之,CSE 作为一种针对登革热病毒 E 蛋白的进入抑制剂表现出抗病毒活性。
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