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nephrin在人类肾发生中细胞连接形成中的作用。

Role of nephrin in cell junction formation in human nephrogenesis.

作者信息

Ruotsalainen V, Patrakka J, Tissari P, Reponen P, Hess M, Kestilä M, Holmberg C, Salonen R, Heikinheimo M, Wartiovaara J, Tryggvason K, Jalanko H

机构信息

Biocenter and Department of Biochemistry, University of Oulu, Oulu, Finland. University of Helsinki, Finland.

出版信息

Am J Pathol. 2000 Dec;157(6):1905-16. doi: 10.1016/S0002-9440(10)64829-8.

Abstract

Nephrin is a cell adhesion protein located at the slit diaphragm area of glomerular podocytes. Mutations in nephrin-coding gene (NPHS1) cause congenital nephrotic syndrome (NPHS1). We studied the developmental expression of nephrin, ZO-1 and P-cadherin in normal fetal kidneys and in NPHS1 kidneys. We used in situ hybridization and immunohistochemistry at light and electron microscopic levels. Nephrin and zonula occludens-1 (ZO-1) were first expressed in late S-shaped bodies. During capillary loop stage, nephrin and ZO-1 localized at the basal margin and in the cell-cell adhesion sites between developing podocytes, especially in junctions with ladder-like structures. In mature glomeruli, nephrin and ZO-1 concentrated at the slit diaphragm area. P-cadherin was first detected in ureteric buds, tubules, and vesicle stage glomeruli. Later, P-cadherin was seen at the basal margin of developing podocytes. Fetal NPHS1 kidneys with Fin-major/Fin-major genotype did not express nephrin, whereas the expression of ZO-1 and P-cadherin was comparable to that of control kidneys. Although early junctional complexes proved structurally normal, junctions with ladder-like structures and slit diaphragms were completely missing. The results indicate that nephrin is dispensable for early development of podocyte junctional complexes. However, nephrin appears to be essential for formation of junctions with ladder-like structures and slit diaphragms.

摘要

Nephrin是一种位于肾小球足细胞裂孔隔膜区域的细胞粘附蛋白。Nephrin编码基因(NPHS1)的突变会导致先天性肾病综合征(NPHS1)。我们研究了Nephrin、ZO-1和P-钙黏蛋白在正常胎儿肾脏和NPHS1肾脏中的发育表达情况。我们在光镜和电镜水平上使用了原位杂交和免疫组织化学方法。Nephrin和紧密连接蛋白1(ZO-1)最初在晚期S形小体中表达。在毛细血管袢阶段,Nephrin和ZO-1定位于发育中的足细胞的基底边缘以及细胞间粘附部位,特别是在具有梯状结构的连接处。在成熟肾小球中,Nephrin和ZO-1集中在裂孔隔膜区域。P-钙黏蛋白最初在输尿管芽、肾小管和囊状期肾小球中被检测到。后来,在发育中的足细胞的基底边缘可见P-钙黏蛋白。具有Fin-major/Fin-major基因型的胎儿NPHS1肾脏不表达Nephrin,而ZO-1和P-钙黏蛋白的表达与对照肾脏相当。尽管早期连接复合体在结构上被证明是正常的,但具有梯状结构和裂孔隔膜的连接处却完全缺失。结果表明,Nephrin对于足细胞连接复合体的早期发育并非必需。然而,Nephrin似乎对于具有梯状结构和裂孔隔膜的连接处的形成至关重要。

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