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腔液流动对 3D 可灌注肾皮质集合管模型中 mpkCCD 细胞穹顶形成的影响。

Effect of luminal flow on doming of mpkCCD cells in a 3D perfusable kidney cortical collecting duct model.

机构信息

Division of Nephrology, Department of Medicine, Icahn School of Medicine at Mount Sinai, New York, New York.

Division of Pediatric Nephrology and Hypertension, Department of Pediatrics, Icahn School of Medicine at Mount Sinai, New York, New York.

出版信息

Am J Physiol Cell Physiol. 2020 Jul 1;319(1):C136-C147. doi: 10.1152/ajpcell.00405.2019. Epub 2020 May 13.

Abstract

The cortical collecting duct (CCD) of the mammalian kidney plays a major role in the maintenance of total body electrolyte, acid/base, and fluid homeostasis by tubular reabsorption and excretion. The mammalian CCD is heterogeneous, composed of Na-absorbing principal cells (PCs) and acid-base-transporting intercalated cells (ICs). Perturbations in luminal flow rate alter hydrodynamic forces to which these cells in the cylindrical tubules are exposed. However, most studies of tubular ion transport have been performed in cell monolayers grown on or epithelial sheets affixed to a flat support, since analysis of transepithelial transport in native tubules by in vitro microperfusion requires considerable expertise. Here, we report on the generation and characterization of an in vitro, perfusable three-dimensional kidney CCD model (3D CCD), in which immortalized mouse PC-like mpkCCD cells are seeded within a cylindrical channel embedded within an engineered extracellular matrix and subjected to luminal fluid flow. We find that a tight epithelial barrier composed of differentiated and polarized PCs forms within 1 wk. Immunofluorescence microscopy reveals the apical epithelial Na channel ENaC and basolateral Na/K-ATPase. On cessation of luminal flow, benzamil-inhibitable cell doming is observed within these 3D CCDs consistent with the presence of ENaC-mediated Na absorption. Our 3D CCD provides a geometrically and microphysiologically relevant platform for studying the development and physiology of renal tubule segments.

摘要

哺乳动物肾脏的皮质集合管 (CCD) 通过肾小管重吸收和排泄,在维持全身电解质、酸碱和液体平衡方面发挥着重要作用。哺乳动物 CCD 是异质的,由钠吸收主细胞 (PC) 和酸碱转运的闰细胞 (IC) 组成。管腔内流速的改变会改变这些圆柱状小管中的细胞所暴露的流体动力。然而,大多数关于管状离子转运的研究都是在单层细胞上进行的,这些细胞生长在平面支持物上或贴附在平面支持物上,因为通过体外微灌注分析天然小管中的跨上皮转运需要相当多的专业知识。在这里,我们报告了一种体外可灌注的三维肾脏 CCD 模型 (3D CCD) 的生成和特性,其中永生的小鼠 PC 样 mpkCCD 细胞被播种在一个圆柱形通道内,该通道嵌入在工程细胞外基质中,并受到管腔内流体流动的影响。我们发现,由分化和极化的 PC 组成的紧密上皮屏障在 1 周内形成。免疫荧光显微镜显示顶端上皮钠通道 ENaC 和基底外侧的 Na/K-ATPase。在停止管腔内流动时,这些 3D CCD 中观察到苯甲脒抑制的细胞穹顶,这与 ENaC 介导的钠吸收的存在一致。我们的 3D CCD 为研究肾小管段的发育和生理学提供了一个几何形状和微生理学上相关的平台。

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