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功能性 Fc 受体和额外免疫复合物受体在小鼠肾细胞上的差异表达。

Differential expression of functional Fc-receptors and additional immune complex receptors on mouse kidney cells.

机构信息

Department of Pediatrics, Renal Section, Baylor College of Medicine, Houston, TX, United States.

出版信息

Mol Immunol. 2013 Dec;56(4):369-79. doi: 10.1016/j.molimm.2013.05.219. Epub 2013 Aug 1.

DOI:10.1016/j.molimm.2013.05.219
PMID:23911392
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3799920/
Abstract

The precise mechanisms by which circulating immune complexes accumulate in the kidney to form deposits in glomerulonephritis are not well understood. In particular, the role of resident cells within glomeruli of the kidney has been widely debated. Immune complexes have been shown to bind one glomerular cell type (mesangial cells) leading to functional responses such as pro-inflammatory cytokine production. To further assess the presence of functional immunoreceptors on resident glomerular cells, cultured mouse renal epithelial, endothelial, and mesangial cells were treated with heat-aggregated mouse IgG or preformed murine immune complexes. Mesangial and renal endothelial cells were found to bind IgG complexes, whereas glomerular epithelial cell binding was minimal. A blocking antibody for Fc-gamma receptors reduced binding to mesangial cells but not renal endothelial cells, suggesting differential immunoreceptor utilization. RT-PCR and immunostaining based screening of cultured renal endothelial cells showed limited low-level expression of known Fc-receptors and Ig binding proteins. The interaction between mesangial cells and renal endothelial cells and immune complexes resulted in distinct, cell-specific patterns of chemokine and cytokine production. This novel pathway involving renal endothelial cells likely contributes to the predilection of circulating immune complex accumulation within the kidney and to the inflammatory responses that drive kidney injury.

摘要

循环免疫复合物在肾脏中积累并形成沉积物的精确机制尚不清楚。特别是,肾脏肾小球内固有细胞的作用一直存在广泛争议。免疫复合物已被证明可以结合一种肾小球细胞类型(系膜细胞),导致功能性反应,如促炎细胞因子的产生。为了进一步评估固有肾小球细胞上功能性免疫受体的存在,培养的小鼠肾上皮细胞、内皮细胞和系膜细胞用热聚集的小鼠 IgG 或预先形成的小鼠免疫复合物处理。发现系膜细胞和肾内皮细胞能够结合 IgG 复合物,而肾小球上皮细胞的结合则很少。针对 Fc-γ 受体的阻断抗体减少了与系膜细胞的结合,但不减少与肾内皮细胞的结合,表明免疫受体的利用存在差异。基于 RT-PCR 和免疫染色的培养肾内皮细胞筛选显示,已知的 Fc 受体和 Ig 结合蛋白的表达水平有限。系膜细胞和肾内皮细胞与免疫复合物的相互作用导致趋化因子和细胞因子产生的独特的细胞特异性模式。这种涉及肾内皮细胞的新途径可能有助于循环免疫复合物在肾脏内的积累,并有助于驱动肾脏损伤的炎症反应。

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本文引用的文献

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