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睫状神经营养因子在体外与受体的结合:形成白细胞介素-6型六聚体复合物的证据。

In vitro binding of ciliary neurotrophic factor to its receptors: evidence for the formation of an IL-6-type hexameric complex.

作者信息

De Serio A, Graziani R, Laufer R, Ciliberto G, Paonessa G

机构信息

Istituto di Ricerche di Biologia Molecolare, Roma, Italy.

出版信息

J Mol Biol. 1995 Dec 15;254(5):795-800. doi: 10.1006/jmbi.1995.0655.

Abstract

Ciliary neurotrophic factor (CNTF) is a cytokine sharing structural and functional similarities with interleukin-6 (IL-6) and other helical cytokines that utilize the common signalling chain gp130. While IL-6 induces gp130 dimerization, CNTF, after the initial interaction with the specific, non-signalling receptor subunit, CNTFR, induces the formation of gp130/LIF-receptor heterodimers. Through immunoprecipitation experiments with tagged soluble receptor molecules, we recently demonstrated that IL-6 drives the formation of a hexameric receptor complex with a defined topology and composed of two IL-6, two IL-6R alpha and two gp130 molecules. Here, we apply the same strategy to study the assembly in vitro of the CNTF receptor complex. We present evidence that both the cytokine and the specific binding chain undergo dimerization in the presence of gp130. Furthermore, although gp130 and LIFR are able to bind independently to the CNTF/CNTFR sub-complex, they never form homodimers but only heterodimers. We propose that CNTF assembles a hexameric receptor complex composed of two CNTF, two CNTFR, one gp130 and one LIFR molecule, and present a model of the reciprocal interaction of these molecules based on similarities with the IL-6 hexameric complex.

摘要

睫状神经营养因子(CNTF)是一种细胞因子,与白细胞介素-6(IL-6)以及其他利用共同信号链gp130的螺旋细胞因子在结构和功能上具有相似性。IL-6可诱导gp130二聚化,而CNTF在与特异性非信号受体亚基CNTFR发生初始相互作用后,会诱导gp130/白血病抑制因子受体(LIFR)异二聚体的形成。通过用带标签的可溶性受体分子进行免疫沉淀实验,我们最近证明IL-6驱动形成具有特定拓扑结构且由两个IL-6、两个IL-6Rα和两个gp130分子组成的六聚体受体复合物。在此,我们应用相同策略来研究CNTF受体复合物的体外组装。我们提供的证据表明,在gp130存在的情况下,细胞因子和特异性结合链都会发生二聚化。此外,尽管gp130和LIFR能够独立结合到CNTF/CNTFR亚复合物上,但它们从不形成同二聚体,而只形成异二聚体。我们提出CNTF组装成一个由两个CNTF、两个CNTFR、一个gp130和一个LIFR分子组成的六聚体受体复合物,并基于与IL-6六聚体复合物的相似性,给出了这些分子相互作用的模型。

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