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人胎儿肾脏中发育肾小球的免疫组织化学研究。

An immunohistochemical study of developing glomeruli in human fetal kidneys.

作者信息

Naruse K, Fujieda M, Miyazaki E, Hayashi Y, Toi M, Fukui T, Kuroda N, Hiroi M, Kurashige T, Enzan H

机构信息

First Department of Pathology and Department of Pediatrics, Kochi Medical School, Kochi, Japan.

出版信息

Kidney Int. 2000 May;57(5):1836-46. doi: 10.1046/j.1523-1755.2000.00033.x.

Abstract

BACKGROUND

In the glomerulonephritis, mesenchymal cells frequently repeat the expression of fetal immunohistochemical phenotypes. However, in human glomerulogenesis the phenotypic alteration of mesangial and other types of glomerular cells has not been clearly defined. Our aim was to clarify the characteristics of fetal mesangial cells and glomerular capillary endothelial cells, as well as their changes during glomerulogenesis using immunohistochemistry.

METHODS

We examined the renal tissues of 34 autopsied fetuses and neonates, 5 children, and 5 adults using immunohistochemistry and immunoelectron microscopy, using antibodies for cytoskeletons, contraction-associated proteins, and endothelial cell markers.

RESULTS

In the V and S stages, there were no cells showing mesangial and endothelial features within the vesicles and the S-shaped bodies. In the S stage, small blood vessels, consisting of endothelial cells (CD31+, CD34+) and primitive perivascular mesenchymal cells (alpha-smooth muscle actin+, low molecular caldesmon+, vimentin+), were branched from developing interlobular arteries and appeared to extend to the lower clefts of the S-shaped bodies. In the C stage, the perivascular mesenchymal cells aggregated at the root of the immature glomeruli. In the M stage, they migrated toward the periphery of immature glomeruli and gradually lost their fetal immunohistochemical features. Similarly, with further maturation, the fetal glomerular capillary endothelial cells gradually lost the immunostaining for CD34, while the strong staining intensity of CD31 remained unchanged, just as that in the adult glomerular capillary endothelial cells.

CONCLUSIONS

In human glomerulogenesis, we demonstrate that fetal mesangial and capillary endothelial cells change their immunohistochemical phenotypes with maturation. They gradually lose fetal immunohistochemical phenotypes. Already before birth, the mesangial cells in almost all glomeruli at the late M stage acquire the adult phenotype.

摘要

背景

在肾小球肾炎中,间充质细胞常重现胎儿免疫组化表型的表达。然而,在人类肾小球发生过程中,系膜细胞和其他类型肾小球细胞的表型改变尚未明确界定。我们的目的是利用免疫组化阐明胎儿系膜细胞和肾小球毛细血管内皮细胞的特征,以及它们在肾小球发生过程中的变化。

方法

我们使用针对细胞骨架、收缩相关蛋白和内皮细胞标志物的抗体,通过免疫组化和免疫电子显微镜检查了34例尸检胎儿和新生儿、5例儿童及5例成人的肾组织。

结果

在V期和S期,囊泡和S形体中未发现具有系膜和内皮特征的细胞。在S期,由内皮细胞(CD31+、CD34+)和原始血管周围间充质细胞(α平滑肌肌动蛋白+、低分子量钙调蛋白+、波形蛋白+)组成的小血管从发育中的小叶间动脉分支出来,并似乎延伸至S形体的下裂。在C期,血管周围间充质细胞聚集在未成熟肾小球的根部。在M期,它们向未成熟肾小球的周边迁移,并逐渐失去其胎儿免疫组化特征。同样,随着进一步成熟,胎儿肾小球毛细血管内皮细胞逐渐失去CD34免疫染色,而CD31的强染色强度保持不变,与成人肾小球毛细血管内皮细胞相同。

结论

在人类肾小球发生过程中,我们证明胎儿系膜细胞和毛细血管内皮细胞随着成熟而改变其免疫组化表型。它们逐渐失去胎儿免疫组化表型。在出生前,晚期M期几乎所有肾小球中的系膜细胞已获得成人表型。

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