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足细胞有助于肾小球新月体的形成。

Podocytes contribute to the formation of glomerular crescents.

作者信息

Thorner Paul S, Ho Michael, Eremina Vera, Sado Yoshikazu, Quaggin Susan

机构信息

Division of Pathology, Hospital for Sick Children, 555 University Avenue, Toronto, Ontario M5G 1X8, Canada.

出版信息

J Am Soc Nephrol. 2008 Mar;19(3):495-502. doi: 10.1681/ASN.2006101115. Epub 2008 Jan 16.

Abstract

The cellular composition of crescents in glomerular disease is controversial. The role of podocytes in crescent formation has been especially difficult to study because podocytes typically lose their characteristic terminally differentiated phenotype under disease conditions, making them difficult to identify. We reasoned that the intermediate filament protein nestin, a marker of progenitor cells that has recently been identified in podocytes, may allow the investigation of podocyte involvement in glomerular crescents. In a series of 35 biopsies with crescentic glomerular disease, all showed nestin-positive cells in the crescents, ranging in number from occasional to approximately 50% of crescent cells. Other podocyte markers, such as podocin and WT1, failed to identify cells in crescents, and no contribution by endothelial or myogenic cells was noted. CD68-positive cells were observed in 80% of cases but were never as numerous as the nestin-positive cells. Nestin and CD68 were not coexpressed by the same cells, providing no evidence of trans-differentiation of podocytes into a macrophage phenotype. Keratin-positive cells were found in crescents in 51% of cases, but only as occasional cells. Up to one third of crescent cells were cycling in 48% of biopsies, and double immunostaining identified these cells as a mixture of nestin-positive cells and "null" cells (negative for nestin, CD68, and keratin). In addition to our observations in human disease, we also identified nestin-positive proliferating podocytes in the crescents of 2 mouse models of crescentic glomerulonephritis. We conclude that podocytes play a role in the formation of glomerular crescents.

摘要

肾小球疾病中新月体的细胞组成存在争议。足细胞在新月体形成中的作用一直特别难以研究,因为足细胞在疾病状态下通常会失去其特征性的终末分化表型,难以识别。我们推断,中间丝蛋白巢蛋白(一种最近在足细胞中被鉴定出的祖细胞标志物)可能有助于研究足细胞在肾小球新月体中的作用。在一系列35例新月体性肾小球疾病活检中,所有病例的新月体中均显示有巢蛋白阳性细胞,数量从偶尔出现到约占新月体细胞的50%不等。其他足细胞标志物,如足动蛋白和WT1,未能识别出新月体中的细胞,也未发现内皮细胞或肌源性细胞的贡献。80%的病例中观察到CD68阳性细胞,但数量从未超过巢蛋白阳性细胞。巢蛋白和CD68并非由同一细胞共表达,这表明没有证据支持足细胞向巨噬细胞表型的转分化。51%的病例中在新月体中发现了角蛋白阳性细胞,但只是偶尔出现。在48%的活检中,多达三分之一的新月体细胞处于增殖状态,双重免疫染色将这些细胞鉴定为巢蛋白阳性细胞和“无标记”细胞(巢蛋白、CD68和角蛋白均为阴性)的混合物。除了在人类疾病中的观察结果外,我们还在两种新月体性肾小球肾炎小鼠模型的新月体中鉴定出了巢蛋白阳性的增殖足细胞。我们得出结论,足细胞在肾小球新月体的形成中起作用。

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