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首页> 外文期刊>Angewandte Chemie >Membrane Deformation by Neolectins with Engineered Glycolipid Binding Sites
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Membrane Deformation by Neolectins with Engineered Glycolipid Binding Sites

机译:Neolectins具有工程化的糖脂结合位点的膜变形。

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摘要

Lectins are glycan-binding proteins that are involved in the recognition of glycoconjugales at the cell surface. When binding to glycolipids, multivalent lectins can affect their distribution and alter membrane shapes. Neolectins have now been designed with controlled number and position of binding sites to decipher the role of multivalency on avidity to a glycosylated surface and on membrane dynamics of glycolipids. A monomeric hexavalent neolectin has been first engineered from a trimeric hexavalent bacterial lectin, From this neolectin template, 13 different neolectins with a valency ranging from 0 to 6 were designed, produced, and analyzed for their ability to bind fucose in solution, to attach to a glycosylated surface and to invaginate glycolipid-conlaining giant liposomes. Whereas the avidity only depends on the presence of at least two binding sites, the ability to bend and invaginate membranes critically depends on the distance between two adjacent binding sites.
机译:凝集素是聚糖结合蛋白,参与细胞表面糖缀合物的识别。当与糖脂结合时,多价凝集素会影响其分布并改变膜的形状。现在已经设计了具有控制的结合位点数目和位置的新凝集素,以解释多价对糖基化表面的亲和力和糖脂膜动力学的作用。首先从三聚体六价细菌凝集素中工程化了单体六价新凝集素。从该新凝集素模板中,设计,生产了13种价数范围为0至6的不同新凝集素,并分析了它们与溶液中岩藻糖结合的能力。糖基化的表面并掺入糖脂相关的巨型脂质体。亲合力仅取决于至少两个结合位点的存在,而弯曲和向内翻膜的能力关键取决于两个相邻结合位点之间的距离。

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