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解析壳聚糖基肝素硫酸盐模拟物与生长因子结合的结构景观:揭示结构决定因素以实现最佳活性。

Unraveling the Structural Landscape of Chitosan-Based Heparan Sulfate Mimics Binding to Growth Factors: Deciphering Structural Determinants for Optimal Activity.

机构信息

Departamento de Química Bio-Orgánica, Instituto de Química Orgánica General (IQOG-CSIC), CSIC, Juan de la Cierva 3, 28006 Madrid, Spain.

Departamento de Química en Ciencias Farmacéuticas, Facultad de Farmacia, Universidad Complutense de Madrid, Plaza de Ramón y Cajal, s/n, 28040 Madrid, Spain.

出版信息

ACS Appl Mater Interfaces. 2020 Jun 10;12(23):25534-25545. doi: 10.1021/acsami.0c03074. Epub 2020 Jun 1.

DOI:10.1021/acsami.0c03074
PMID:32426965
Abstract

Chitosan sulfates have demonstrated the ability to mimic heparan sulfate (HS) function. In this context, it is crucial to understand how the specific structural properties of HS domains determine their functionalities and biological activities. In this study, several HS-mimicking chitosans have been prepared to mimic the structure of HS domains that have proved to be functionally significant in cell processes. The results presented herein are in concordance with the hypothesis that sulfated chitosan-growth factor (GF) interactions are controlled by a combination of two effects: the electrostatic interactions and the conformational adaptation of the polysaccharide. Thus, we found that highly charged -sulfated and polysaccharides with a low degree of contraction interacted more strongly with GFs than -sulfated , with a higher degree of contraction and a low charge. Finally, the evidence gathered suggests that would be able to bind to an allosteric zone and is likely to enhance GF signaling activity. This is because the bound protein remains able to bind to its cognate receptor, promoting an effect on cell proliferation as has been shown for PC12 cells. However, and would sequester the protein, decreasing the GF signaling activity by depleting the protein or locally blocking its active site.

摘要

壳聚糖硫酸盐已被证明具有模拟肝素硫酸盐 (HS) 功能的能力。在这种情况下,了解 HS 结构域的特定结构特性如何决定其功能和生物活性至关重要。在这项研究中,已经制备了几种模拟 HS 结构域的壳聚糖,以模拟在细胞过程中被证明具有功能重要性的 HS 结构域。本文提出的结果与以下假设一致,即带负电荷的壳聚糖-生长因子 (GF) 相互作用受两种效应的共同控制:静电相互作用和多糖的构象适应性。因此,我们发现,与具有高收缩度和低电荷的 -硫酸化多糖相比,高电荷的 -硫酸化多糖与 GF 相互作用更强。最后,收集到的证据表明, 将能够与别构区结合,并且可能增强 GF 信号转导活性。这是因为结合的蛋白质仍然能够与其同源受体结合,如对 PC12 细胞的研究所示,促进细胞增殖的作用。然而, 和 会隔离蛋白质,通过耗尽蛋白质或局部阻断其活性位点来降低 GF 信号转导活性。

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