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肾毒性血清性肾炎大鼠肾小球细胞培养物中白细胞介素1的产生

Production of interleukin 1 in glomerular cell cultures from rats with nephrotoxic serum nephritis.

作者信息

Matsumoto K, Hatano M

机构信息

Second Department of Internal Medicine, Nihon University School of Medicine, Tokyo, Japan.

出版信息

Clin Exp Immunol. 1989 Jan;75(1):123-8.

Abstract

To investigate the role of cytokines in the pathogenesis of experimental glomerulonephritis (GN), we examined interleukin 1 (IL-1) activity in isolated glomeruli of rats with an accelerated autologous form of nephrotoxic serum nephritis (NTSN). Glomeruli were isolated and explanted in tissue culture. The prominent feature of the glomerular outgrowth of the glomeruli in the NTSN was the presence of large numbers of type III cells (macrophages). In addition, there were significantly greater numbers of type II (mesangial) cells in culture from the NTSN rats as compared with glomeruli from normal rats, though the numbers of type I (epithelial) cells were the same. IL-1 bioactivity was significantly higher in culture supernatants generated by glomeruli isolated from NTSN animals versus normal animals early in the course of the disease. When glomerular culture supernatants and purified IL-1 were pre-incubated with an anti-IL-1 beta antibody, a parallel decrease of the biological activity was found, suggesting that the biologically active binding sites of the culture supernatants and monocyte-produced IL-1 share some common structure. The administration of a rabbit anti-rat macrophage serum (AMS) prevented the outgrowths of type III cells (macrophages) and type II (mesangial) cells and reduced the production of IL-1 activity in the NTSN rats. In this experimental model IL-1 synthesis, probably by multiple cell types, is present early in the disease process and perhaps may be an important mediator of glomerular immune injury.

摘要

为了研究细胞因子在实验性肾小球肾炎(GN)发病机制中的作用,我们检测了加速型自体肾毒性血清性肾炎(NTSN)大鼠分离肾小球中的白细胞介素1(IL-1)活性。分离肾小球并将其植入组织培养中。NTSN大鼠肾小球生长的突出特征是存在大量III型细胞(巨噬细胞)。此外,与正常大鼠的肾小球相比,NTSN大鼠培养的II型(系膜)细胞数量明显更多,而I型(上皮)细胞数量相同。在疾病早期,与正常动物相比,从NTSN动物分离的肾小球产生的培养上清液中的IL-1生物活性显著更高。当肾小球培养上清液和纯化的IL-1与抗IL-1β抗体预孵育时,发现生物活性平行下降,这表明培养上清液和单核细胞产生的IL-1的生物活性结合位点具有一些共同结构。给予兔抗大鼠巨噬细胞血清(AMS)可阻止III型细胞(巨噬细胞)和II型(系膜)细胞的生长,并降低NTSN大鼠中IL-1活性的产生。在这个实验模型中,IL-1的合成可能由多种细胞类型在疾病过程早期进行,并且可能是肾小球免疫损伤的重要介质。

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