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从人尿中纯化至同质的肿瘤坏死因子结合蛋白可保护细胞免受肿瘤坏死因子毒性的影响。

A tumor necrosis factor-binding protein purified to homogeneity from human urine protects cells from tumor necrosis factor toxicity.

作者信息

Engelmann H, Aderka D, Rubinstein M, Rotman D, Wallach D

机构信息

Department of Virology, Weizmann Institute of Science, Rehovot, Israel.

出版信息

J Biol Chem. 1989 Jul 15;264(20):11974-80.

PMID:2545693
Abstract

Unfractionated preparations of the proteins of human urine provided protection against the in vitro cytocidal effect of tumor necrosis factor (TNF). In certain cells, the proteins decreased expression of the receptors for TNF in a temperature-dependent way. In all cells examined, the proteins were found to interfere also with the binding of both TNF and interleukin-1 when applied directly into the binding assays. That effect could be observed in the cold, suggesting that it was independent of cellular metabolism. A protein which protects cells against the cytotoxicity of TNF was purified from human urine by chromatography on CM-Sepharose followed by high performance liquid chromatography on Mono Q and Mono S columns and reversed phase high performance liquid chromatography. This protein is a very minor constituent of normal urine, with an apparent molecular weight of about 27,000 in sodium dodecyl sulfate-polyacrylamide gel electrophoresis under both reducing and nonreducing conditions. Homogeneity of the purified protein was confirmed by microsequence analysis which revealed a single N-terminal sequence: Asp-Ser-Val-Cys-Pro-. The protein protected cells from TNF toxicity at concentrations of a few nanograms per ml and interfered with the binding of both TNF-alpha and TNF-beta to cells, when applied simultaneously with the cytokines. However, unlike crude preparations of the urinary proteins, the purified protein did not induce in cells a decrease in ability to bind TNF nor did it interfere with the binding of interleukin-1 to its receptor. Direct, specific binding to the protein of TNF-alpha and, to a lesser extent, also TNF-beta, but not of interleukin-1 nor interferon-gamma could be demonstrated. It is suggested that this protein blocks the function of TNF by competing for TNF with the TNF receptor and not by interacting with the target cell.

摘要

人尿蛋白的未分级制剂可保护细胞免受肿瘤坏死因子(TNF)的体外杀细胞作用。在某些细胞中,这些蛋白质以温度依赖的方式降低了TNF受体的表达。在所检测的所有细胞中,当直接应用于结合试验时,这些蛋白质还会干扰TNF和白细胞介素-1的结合。在低温下可观察到这种效应,这表明它与细胞代谢无关。通过在CM-琼脂糖凝胶上进行层析,然后在Mono Q和Mono S柱上进行高效液相色谱以及反相高效液相色谱,从人尿中纯化出一种保护细胞免受TNF细胞毒性作用的蛋白质。这种蛋白质是正常尿液中的一种微量成分,在还原和非还原条件下的十二烷基硫酸钠-聚丙烯酰胺凝胶电泳中,其表观分子量约为27,000。通过微序列分析证实了纯化蛋白质的均一性,该分析揭示了一个单一的N端序列:天冬氨酸-丝氨酸-缬氨酸-半胱氨酸-脯氨酸-。当与细胞因子同时应用时,该蛋白质在每毫升几纳克的浓度下就能保护细胞免受TNF毒性作用,并干扰TNF-α和TNF-β与细胞的结合。然而,与尿蛋白的粗制品不同,纯化后的蛋白质不会诱导细胞结合TNF的能力下降,也不会干扰白细胞介素-1与其受体的结合。可以证明TNF-α能直接、特异性地与该蛋白质结合,TNF-β的结合程度稍低,但白细胞介素-1和干扰素-γ则不能。有人提出,这种蛋白质通过与TNF受体竞争TNF来阻断TNF的功能,而不是通过与靶细胞相互作用。

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A tumor necrosis factor-binding protein purified to homogeneity from human urine protects cells from tumor necrosis factor toxicity.从人尿中纯化至同质的肿瘤坏死因子结合蛋白可保护细胞免受肿瘤坏死因子毒性的影响。
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