首页> 美国卫生研究院文献>Clinical and Experimental Immunology >Prolonged circulation of immune complexes due to various altered immune functions contributes to nephritis in MRL/lpr mice.
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Prolonged circulation of immune complexes due to various altered immune functions contributes to nephritis in MRL/lpr mice.

机译:由于各种免疫功能改变而导致的免疫复合物循环时间延长导致MRL / lpr小鼠肾炎。

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摘要

To gain some insight into the pathogenesis of proliferative lupus nephritis in MRL/lpr mice we investigated the kinetics of removal of immune complexes from the circulation, the carrier state of blood cells, the uptake of complexes by the mononuclear phagocyte system, and the localization of complexes in kidneys. In nephritic MRL/lpr mice challenged with a subsaturating dose of radiolabelled complexes (2.5 mg bovine serum albumin-anti-bovine serum albumin) liver uptake was profoundly decreased, removal of circulating complexes was delayed, and 12-h kidney localization of complexes was enhanced 7.3-fold, in comparison to control mice. The findings were not encumbered by differences in complement concentration and most likely are attributable to various altered immune functions: spontaneous polyclonal activation of B cells, enhanced production of endogenous immune complexes, delayed removal of complexes from the circulation, and decreased uptake of complexes by the mononuclear phagocyte system. In concert, such altered functions contribute to prolonged circulation of complexes to result in their enhanced deposition in the microcirculation.
机译:为了深入了解增生性狼疮肾炎在MRL / lpr小鼠中的发病机理,我们研究了从循环中清除免疫复合物的动力学,血细胞的携带状态,单核吞噬细胞系统对复合物的摄取以及对单核细胞吞噬的定位。肾脏中的复合物。在亚饱和剂量的放射性标记复合物(2.5 mg牛血清白蛋白-抗牛血清白蛋白)激发的肾病MRL / lpr小鼠中,肝脏摄取显着降低,循环复合物的清除被延迟,并且复合物的12小时肾脏定位增强与对照小鼠相比,是7.3倍。该发现不受补体浓度差异的影响,最可能归因于各种免疫功能的改变:B细胞的自发多克隆激活,内源性免疫复合物的产生增加,复合物从循环中的清除延迟以及复合物的摄取减少。单核吞噬细胞系统。一致地,这种改变的功能有助于延长复合物的循环,从而导致它们在微循环中的沉积增加。

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