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白细胞介素-6 信号转导蛋白 gp130 未配位细胞外结构域在溶液中的结构。

The structure of the unliganded extracellular domain of the interleukin-6 signal transducer gp130 in solution.

机构信息

Institute of Biochemistry, Christian-Albrechts-University Kiel, Olshausenstr. 40, 24098 Kiel, Germany.

出版信息

Eur J Cell Biol. 2011 Jun-Jul;90(6-7):515-20. doi: 10.1016/j.ejcb.2010.09.012. Epub 2010 Oct 30.

DOI:10.1016/j.ejcb.2010.09.012
PMID:21035897
Abstract

Interleukin-6 (IL-6) plays an important role in immune responses and signals via two different pathways. When IL-6 binds to its non-signalling membrane-bound receptor (IL-6R), a non-covalent dimer of the ubiquitous interleukin-6 signal transducer gp130 is recruited to initiate intracellular signalling cascades. This so-called classical signalling pathway is restricted to cells expressing the membrane-bound IL-6R, such as hepatocytes and certain leukocytes. In addition, an alternative trans-signalling pathway uses soluble forms of IL-6R (sIL-6R) in complex with IL-6 to activate cells expressing gp130, but not membrane-bound IL-6R. In both cases, a tetrameric or hexameric signalling complex consisting of two gp130 molecules and one or two molecules each of IL-6 and (s)IL-6R is formed. The structure of the hexameric complex of the ligand-binding domains of gp130 (D1-D3) with IL-6 and sIL-6R has been solved by X-ray crystallography as well as the full-length extracellular part of gp130 (D1-D6) as a monomer. Since gp130 exists as a preformed dimer on the cell surface, we used a sgp130Fc fusion protein - consisting of two extracellular gp130 regions (D1-D6) dimerised by an IgG1-Fc part - to study the structure of unliganded gp130 extracellular domains in solution by small-angle X-ray scattering (SAXS). The SAXS data indicated that sgp130Fc forms a rigid molecule in solution. The low resolution structural model reveals an elongated assembly with an Fc base and two gp130 arms, whereby the orientation of the ligand-binding domains D1-D3 with respect to the membrane-proximal domains D4-D6 differs from that in the crystallographic monomer. Functional implications of these findings are discussed.

摘要

白细胞介素 6(IL-6)通过两条不同的途径在免疫反应和信号转导中发挥重要作用。当 IL-6 与非信号转导的膜结合受体(IL-6R)结合时,普遍存在的白细胞介素 6 信号转导蛋白 gp130 的非共价二聚体被招募来启动细胞内信号级联反应。这种所谓的经典信号通路仅限于表达膜结合型 IL-6R 的细胞,如肝细胞和某些白细胞。此外,替代的转信号通路使用可溶性形式的 IL-6R(sIL-6R)与 IL-6 形成复合物来激活表达 gp130 的细胞,但不激活表达膜结合型 IL-6R 的细胞。在这两种情况下,都会形成由两个 gp130 分子和一个或两个 IL-6 和(s)IL-6R 分子组成的四聚体或六聚体信号复合物。通过 X 射线晶体学已经解决了 gp130(D1-D3)配体结合域与 IL-6 和 sIL-6R 的六聚体复合物的结构,以及 gp130 的全长细胞外部分(D1-D6)作为单体的结构。由于 gp130 存在于细胞表面的预先形成的二聚体上,我们使用了一个 sgp130Fc 融合蛋白——由两个细胞外 gp130 区域(D1-D6)通过 IgG1-Fc 部分二聚化组成——通过小角度 X 射线散射(SAXS)研究溶液中非配体结合的 gp130 细胞外结构域的结构。SAXS 数据表明 sgp130Fc 在溶液中形成刚性分子。低分辨率结构模型揭示了一种拉长的组装体,具有一个 Fc 基和两个 gp130 臂,其中配体结合域 D1-D3 相对于膜近端域 D4-D6 的取向与晶体学单体中的不同。讨论了这些发现的功能意义。

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