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Fas抗原和Bcl-2在人类肾小球肾炎中的表达

Expression of Fas antigen and Bcl-2 in human glomerulonephritis.

作者信息

Takemura T, Murakami K, Miyazato H, Yagi K, Yoshioka K

机构信息

Department of Pediatrics, Kinki University School of Medicine, Osaka-sayama, Japan.

出版信息

Kidney Int. 1995 Dec;48(6):1886-92. doi: 10.1038/ki.1995.487.

DOI:10.1038/ki.1995.487
PMID:8587248
Abstract

To understand the regulatory mechanism of apoptosis in human glomerulonephritis, we examined the expression of Fas antigen (CD95) and Bcl-2 in five normal human kidney specimens and 80 tissues from patients with several types of glomerular diseases. These proteins were detected in glomeruli by immunofluorescence. The number of intraglomerular cells positive for Fas antigen was high in Henoch-Schönlein purpura nephritis and lupus nephritis, and that of Bcl-2-positive intraglomerular cells was high in lupus nephritis, focal glomerular sclerosis, and IgA nephritis. Dual-labeling and staining on serial sections indicated that mesangial cells and occasionally infiltrating leukocytes expressed Fas antigen and Bcl-2. In situ hybridization detected Bcl-2 mRNA in glomerular cells. Electron microscopy revealed apoptotic cells and apoptotic bodies in proliferated mesangial areas and within the glomerular capillaries. Fragmented DNA was detected in glomeruli by in situ nick end labeling, the data of which paralleled the number of Fas antigen-positive intraglomerular cells. In mesangial proliferative types of glomerulonephritis, the population of Bcl-2-positive intraglomerular cells, but not that of Fas antigen-positive cells, was significantly correlated with the number of proliferating cell nuclear antigen-positive glomerular cells, the grade of mesangial cell increase, and the magnitude of proteinuria. This study showed that Fas antigen and Bcl-2 are up-regulated in the glomeruli of several types of human renal diseases. Bcl-2 overexpression might play a role in the prolonged proliferation of mesangial cells and glomerular hypercellularity in glomerulonephritis.

摘要

为了解人肾小球肾炎中细胞凋亡的调控机制,我们检测了5例正常人类肾脏标本以及80例患有几种类型肾小球疾病患者的组织中Fas抗原(CD95)和Bcl-2的表达。通过免疫荧光在肾小球中检测到了这些蛋白。Fas抗原阳性的肾小球内细胞数量在过敏性紫癜性肾炎和狼疮性肾炎中较高,而Bcl-2阳性的肾小球内细胞数量在狼疮性肾炎、局灶性肾小球硬化症和IgA肾病中较高。连续切片的双重标记和染色表明,系膜细胞以及偶尔浸润的白细胞表达Fas抗原和Bcl-2。原位杂交在肾小球细胞中检测到了Bcl-2 mRNA。电子显微镜显示在增生的系膜区域和肾小球毛细血管内有凋亡细胞和凋亡小体。通过原位缺口末端标记在肾小球中检测到了DNA片段化,其数据与Fas抗原阳性的肾小球内细胞数量平行。在系膜增生性肾小球肾炎类型中,Bcl-2阳性的肾小球内细胞数量,而非Fas抗原阳性细胞数量,与增殖细胞核抗原阳性的肾小球细胞数量、系膜细胞增加的程度以及蛋白尿的严重程度显著相关。本研究表明,Fas抗原和Bcl-2在几种类型的人类肾脏疾病的肾小球中上调。Bcl-2的过度表达可能在肾小球肾炎中系膜细胞的长期增殖和肾小球细胞增多中起作用。

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