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抑瘤素M/白细胞介素-31共享受体可溶性形式的分子与功能特征

Molecular and functional characterization of a soluble form of oncostatin M/interleukin-31 shared receptor.

作者信息

Diveu Caroline, Venereau Emilie, Froger Josy, Ravon Elisa, Grimaud Linda, Rousseau François, Chevalier Sylvie, Gascan Hugues

机构信息

Institut National de la Santé et de la Recherche Médicale, U564, F-49033 Angers, France.

出版信息

J Biol Chem. 2006 Dec 1;281(48):36673-82. doi: 10.1074/jbc.M607005200. Epub 2006 Oct 6.

Abstract

Activation of the signaling transduction pathways mediated by oncostatin M (OSM) requires the binding of the cytokine to either type I OSM receptor (leukemia inhibitory factor receptor/gp130) or to type II OSM receptor (OSMR/gp130). In the present work we have developed an enzyme-linked immunosorbent assay detecting a soluble form of OSMR (sOSMR) secreted by glioblastoma, hepatoma, and melanoma tumor cell lines. sOSMR was also present in sera of healthy individuals, with increased levels in multiple myeloma. Molecular cloning of a corresponding cDNA was carried out, and it encoded for a 70-kDa protein consisting of a half cytokine binding domain containing the canonical WSXWS motif, an immunoglobulin-like domain, and the first half of a second cytokine binding domain with cysteines in fixed positions. Analysis of the soluble receptor distribution revealed a preferential expression in lung, liver, pancreas, and placenta. sOSMR was able to bind OSM and interleukin-31 when associated to soluble gp130 or soluble interleukin-31R, respectively, and to neutralize both cytokine properties. We have also shown that OSM could positively regulate the synthesis of its own soluble receptor in tumor cells.

摘要

抑瘤素M(OSM)介导的信号转导通路的激活需要该细胞因子与I型OSM受体(白血病抑制因子受体/gp130)或II型OSM受体(OSMR/gp130)结合。在本研究中,我们开发了一种酶联免疫吸附测定法,用于检测胶质母细胞瘤、肝癌和黑色素瘤肿瘤细胞系分泌的可溶性OSMR(sOSMR)。sOSMR也存在于健康个体的血清中,在多发性骨髓瘤患者中水平升高。我们进行了相应cDNA的分子克隆,其编码一种70 kDa的蛋白质,该蛋白质由一个包含典型WSXWS基序的半细胞因子结合结构域、一个免疫球蛋白样结构域以及第二个细胞因子结合结构域的前半部分组成,其中半胱氨酸位于固定位置。对可溶性受体分布的分析显示,其在肺、肝、胰腺和胎盘中优先表达。当分别与可溶性gp130或可溶性白细胞介素-31受体结合时,sOSMR能够结合OSM和白细胞介素-31,并中和这两种细胞因子的特性。我们还表明,OSM可以正向调节肿瘤细胞中其自身可溶性受体的合成。

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