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首页> 外文期刊>Biomacromolecules >Glycosidase Inhibition by Multivalent Presentation of Heparan Sulfate Saccharides on Bottlebrush Polymers
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Glycosidase Inhibition by Multivalent Presentation of Heparan Sulfate Saccharides on Bottlebrush Polymers

机译:糖苷酶通过多价呈递硫酸普硫酸乙酰氨酸乙酰醇聚合物抑制作用

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摘要

We report herein the first-time exploration of the attachment of well-defined saccharide units onto a synthetic polymer backbone for the inhibition of a glycosidase. More specifically, glycopolymers endowed with heparan sulfate (HS) disaccharides were established to inhibit the glycosidase, heparanase, with an IC50, value in the low nanomolar range (1.05 +/- 0.02 nm), a thousand-fold amplification over its monovalent counterpart. The monomeric moieties of these glycopolymers were designed in silico to manipulate the well-established glycotope of heparanase into an inhitope. Studies concluded that (1) the glycopolymers are hydrolytic stable toward heparanase, (2) longer polymer length provides greater inhibition, and (3) increased local saccharide density (monoantennary vs diantennary) is negligible due to hindered active site of heparanase. Furthermore, HS oligosaccharide and polysaccharide controls illustrate the enhanced potency of a multivalent scaffold. Overall, the results on these studies of the multivalent presentation of saccharides on bottlebrush polymers serve as the platform for the design of potent glycosidase inhibitors and have potential to be applied to other HS-degrading proteins.
机译:我们在本文中报告了将明确定义的糖单元附着在合成聚合物主链上的第一次探索,用于抑制糖苷酶。更具体地,建立赋予硫酸乙酰乙酸乙酰丙酯(HS)二糖的糖聚合物以抑制糖苷酶,乙酰肝素酶,用IC50,低纳米摩尔(1.05 +/- 0.02nm),在其单价对应上的千倍放大。这些聚甘醇聚合物的单体部分在硅中设计,以操纵普生素酶的良好的糖糖血清素到惰性血清中。结论:(1)(1)甘醇聚合物是水解稳定的甲肝素酶,(2)更长的聚合物长度提供更大的抑制,并且(3)增加局部糖密度(单南纳型Vs Diantennarary)由于肝胰酶的受阻活性位点可忽略不计。此外,HS寡糖和多糖对照说明了多价支架的增强效力。总体而言,这些研究对瓶装聚合物的多价致糖的多价呈递的研究用作有效糖苷酶抑制剂设计的平台,并且具有应用于其他HS降解蛋白质的潜力。

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