首页> 外文期刊>Journal of Molecular Biology >The EM structure of a type I interferon-receptor complex reveals a novel mechanism for cytokine signaling.
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The EM structure of a type I interferon-receptor complex reveals a novel mechanism for cytokine signaling.

机译:I型干扰素受体复合物的EM结构揭示了细胞因子信号转导的新机制。

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摘要

Type I interferons (IFNs) have pleiotropic effects, including antiviral, antiproliferative, and immunomodulatory responses. All type I IFNs bind to a shared receptor consisting of the two transmembrane proteins ifnar1 and ifnar2. We used negative stain electron microscopy to calculate a three-dimensional reconstruction of the ternary complex formed by a triple mutant IFN alpha2 with the ectodomains of ifnar1 and ifnar2. We present a model of the complex obtained by placing atomic models of subunits into the density map of the complex. The complex of IFN alpha2 with its receptor (a class II cytokine receptor) shows structural similarities to the complexes formed by growth hormone and erythropoietin with their receptors (members of the class I cytokine receptor family). Despite different assembly mechanisms, class I and class II cytokine receptors thus appear to initiate signaling through similar arrangements of the receptors induced by the binding of their respective ligands.
机译:I型干扰素(IFN)具有多效作用,包括抗病毒,抗增殖和免疫调节反应。所有的I型IFN都与由两个跨膜蛋白ifnar1和ifnar2组成的共享受体结合。我们使用负染色电子显微镜来计算三维复合物的三维重建,该复合物是由三联突变体IFN alpha2与ifnar1和ifnar2的胞外域形成的。我们提出了通过将亚基的原子模型放入复合物的密度图中获得的复合物模型。 IFN alpha2及其受体(II类细胞因子受体)的复合物显示出与生长激素和促红细胞生成素及其受体(I类细胞因子受体家族成员)形成的复合物的结构相似性。尽管有不同的组装机制,但I类和II类细胞因子受体似乎通过相似的受体配体结合引发的受体相似信号而启动信号传导。

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