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Structure of the quaternary complex of interleukin-2 with its alpha, beta, and gammac receptors.白细胞介素-2与其α、β和γc受体的四元复合物结构。
Science. 2005 Nov 18;310(5751):1159-63. doi: 10.1126/science.1117893.
2
High-affinity CD25-binding IL-2 mutants potently stimulate persistent T cell growth.高亲和力结合CD25的白细胞介素-2突变体可有效刺激T细胞持续生长。
Biochemistry. 2005 Aug 9;44(31):10696-701. doi: 10.1021/bi050436x.
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The structure of interleukin-2 complexed with its alpha receptor.与α受体复合的白细胞介素-2的结构。
Science. 2005 Jun 3;308(5727):1477-80. doi: 10.1126/science.1109745.
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Clathrin-lndependent endocytosis and signalling of interleukin 2 receptors IL-2R endocytosis and signalling.网格蛋白非依赖型内吞作用与白细胞介素2受体的信号传导:IL-2R内吞作用与信号传导
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The quantal theory of how the immune system discriminates between "self and non-self".关于免疫系统如何区分“自我与非自我”的量子理论。
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Structural analysis of IL-10 and Type I interferon family members and their complexes with receptor.白细胞介素-10和I型干扰素家族成员及其与受体复合物的结构分析
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Compensatory energetic mechanisms mediating the assembly of signaling complexes between interleukin-2 and its alpha, beta, and gamma(c) receptors.介导白细胞介素-2与其α、β和γ(c)受体之间信号复合物组装的代偿性能量机制。
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Human IL-21 and IL-4 bind to partially overlapping epitopes of common gamma-chain.人白细胞介素-21和白细胞介素-4与共同γ链的部分重叠表位结合。
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IL-15Ralpha recycles and presents IL-15 In trans to neighboring cells.白细胞介素-15受体α亚基循环利用并将白细胞介素-15反式呈递给邻近细胞。
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白细胞介素-2信号复合物的晶体结构:异源三聚体细胞因子受体的范例

Crystal structure of the IL-2 signaling complex: paradigm for a heterotrimeric cytokine receptor.

作者信息

Stauber Deborah J, Debler Erik W, Horton Patricia A, Smith Kendall A, Wilson Ian A

机构信息

Department of Molecular Biology, The Scripps Research Institute, 10550 North Torrey Pines Road, La Jolla, CA 92037, USA.

出版信息

Proc Natl Acad Sci U S A. 2006 Feb 21;103(8):2788-93. doi: 10.1073/pnas.0511161103. Epub 2006 Feb 13.

DOI:10.1073/pnas.0511161103
PMID:16477002
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1413841/
Abstract

IL-2 is a cytokine that functions as a growth factor and central regulator in the immune system and mediates its effects through ligand-induced hetero-trimerization of the receptor subunits IL-2R alpha, IL-2R beta, and gamma(c). Here, we describe the crystal structure of the trimeric assembly of the human IL-2 receptor ectodomains in complex with IL-2 at 3.0 A resolution. The quaternary structure is consistent with a stepwise assembly from IL-2/IL-2R alpha to IL-2/IL-2R alpha/IL-2R beta to IL-2/IL-2R alpha/IL-2R beta/gamma(c). The IL-2R alpha subunit forms the largest of the three IL-2/IL-2R interfaces, which, together with the high abundance of charge-charge interactions, correlates well with the rapid association rate and high-affinity interaction of IL-2R alpha with IL-2 at the cell surface. Surprisingly, IL-2R alpha makes no contacts with IL-2R beta or gamma(c), and only minor changes are observed in the IL-2 structure in response to receptor binding. These findings support the principal role of IL-2R alpha to deliver IL-2 to the signaling complex and act as regulator of signal transduction. Cooperativity in assembly of the final quaternary complex is easily explained by the extraordinarily extensive set of interfaces found within the fully assembled IL-2 signaling complex, which nearly span the entire length of the IL-2R beta and gamma(c) subunits. Helix A of IL-2 wedges tightly between IL-2R beta and gamma(c) to form a three-way junction that coalesces into a composite binding site for the final gamma(c) recruitment. The IL-2/gamma(c) interface itself exhibits the smallest buried surface and the fewest hydrogen bonds in the complex, which is consistent with its promiscuous use in other cytokine receptor complexes.

摘要

白细胞介素-2(IL-2)是一种细胞因子,在免疫系统中作为生长因子和核心调节因子发挥作用,并通过配体诱导受体亚基IL-2Rα、IL-2Rβ和γ(c)的异源三聚化来介导其效应。在此,我们描述了人IL-2受体胞外域与IL-2形成的三聚体复合物在3.0埃分辨率下的晶体结构。四级结构与从IL-2/IL-2Rα到IL-2/IL-2Rα/IL-2Rβ再到IL-2/IL-2Rα/IL-2Rβ/γ(c)的逐步组装过程一致。IL-2Rα亚基形成了三个IL-2/IL-2R界面中最大的一个,这与大量的电荷-电荷相互作用一起,与IL-2Rα在细胞表面与IL-2的快速结合速率和高亲和力相互作用密切相关。令人惊讶的是,IL-2Rα与IL-2Rβ或γ(c)没有接触,并且在响应受体结合时,IL-2结构中仅观察到微小变化。这些发现支持了IL-2Rα在将IL-2递送至信号复合物并作为信号转导调节因子方面的主要作用。最终四级复合物组装中的协同作用很容易通过在完全组装的IL-2信号复合物中发现的极其广泛的界面集合来解释,这些界面几乎跨越了IL-2Rβ和γ(c)亚基的整个长度。IL-2的螺旋A紧密楔入IL-2Rβ和γ(c)之间,形成一个三向连接,合并成一个用于最终γ(c)募集的复合结合位点。在复合物中,IL-2/γ(c)界面本身显示出最小的埋藏表面积和最少的氢键,这与其在其他细胞因子受体复合物中的广泛使用是一致的。