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Mouse LSECtin as a model for a human Ebola virus receptor

机译:小鼠LSECtin作为人类埃博拉病毒受体的模型

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摘要

The biochemical properties of mouse LSECtin, a glycan-binding receptor that is a member of the C-type lectin family found on sinusoidal endothelial cells, have been investigated. The C-type carbohydrate-recognition domain of mouse LSECtin, expressed in bacteria, has been used in solid-phase binding assays, and a tetramerized form has been used to probe a glycan array. In spite of sequence differences near the glycan-binding sites, the mouse receptor closely mimics the properties of the human receptor, showing high affinity binding to glycans bearing terminal GlcNAcβ1-2Man motifs. Site-directed mutagenesis has been used to confirm that residues near the binding site that differ between the human and the mouse proteins do not affect this binding specificity. Mouse and human LSECtin have been shown to bind Ebola virus glycoprotein with equivalent affinities, and the GlcNAcβ1-2Man disaccharide has been demonstrated to be an effective inhibitor of this interaction. These studies provide a basis for using mouse LSECtin, and knockout mice lacking this receptor, to model the biological properties of the human receptor.
机译:已经研究了小鼠LSECtin(一种在正弦血管内皮细胞上发现的C型凝集素家族成员)中的聚糖结合受体的生化特性。在细菌中表达的小鼠LSECtin的C型碳水化合物识别结构域已用于固相结合测定,四聚体形式已用于探测聚糖阵列。尽管在聚糖结合位点附近存在序列差异,但是小鼠受体紧密模仿人类受体的特性,显示出对具有末端GlcNAcβ1-2Man基序的聚糖的高亲和力结合。定点诱变已被用于确认人和小鼠蛋白之间结合位点附近的残基不影响该结合特异性。小鼠和人LSECtin已显示出以等效亲和力结合埃博拉病毒糖蛋白,并且GlcNAcβ1-2Man二糖已被证明是这种相互作用的有效抑制剂。这些研究为使用小鼠LSECtin和缺乏这种受体的基因敲除小鼠模拟人受体的生物学特性提供了基础。

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