气道上皮细胞中 CFTR 和 ΔF508-CFTR 对内源性 ENaC 功能表达的调节。

Regulation of endogenous ENaC functional expression by CFTR and ΔF508-CFTR in airway epithelial cells.

机构信息

The Children's Hospital of Philadelphia, University of Pennsylvania School of Medicine, Philadelphia, USA.

出版信息

Am J Physiol Lung Cell Mol Physiol. 2011 Jan;300(1):L88-L101. doi: 10.1152/ajplung.00142.2010. Epub 2010 Oct 8.

DOI:10.1152/ajplung.00142.2010

PMID:20935229

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3023291/

Abstract

The functional expression of the epithelial sodium channel (ENaC) appears elevated in cystic fibrosis (CF) airway epithelia, but the mechanism by which this occurs is not clear. We tested the hypothesis that the cystic fibrosis transmembrane conductance regulator (CFTR) alters the trafficking of endogenously expressed human ENaC in the CFBE41o⁻ model of CF bronchial epithelia. Functional expression of ENaC, as defined by amiloride-inhibited short-circuit current (I(sc)) in Ussing chambers, was absent under control conditions but present in CFBE41o⁻ parental and ΔF508-CFTR-overexpressing cells after treatment with 1 μM dexamethasone (Dex) for 24 h. The effect of Dex was mimicked by incubation with the glucocorticoid hydrocortisone but not with the mineralocorticoid aldosterone. Application of trypsin to the apical surface to activate uncleaved, "near-silent" ENaC caused an additional increase in amiloride-sensitive I(sc) in the Dex-treated cells and was without effect in the control cells, suggesting that Dex increased ENaC cell surface expression. In contrast, Dex treatment did not stimulate amiloride-sensitive I(sc) in CFBE41o⁻ cells that stably express wild-type (wt) CFTR. CFBE41o⁻ wt cells also had reduced expression of α- and γ-ENaC compared with parental and ΔF508-CFTR-overexpressing cells. Furthermore, application of trypsin to the apical surface of Dex-treated CFBE41o⁻ wt cells did not stimulate amiloride-sensitive I(sc), suggesting that ENaC remained absent from the surface of these cells even after Dex treatment. We also tested the effect of trafficking-corrected ΔF508-CFTR on ENaC functional expression. Incubation with 1 mM 4-phenylbutyrate synergistically increased Dex-induced ENaC functional expression in ΔF508-CFTR-overexpressing cells. These data support the hypothesis that wt CFTR can regulate the whole cell, functional, and surface expression of endogenous ENaC in airway epithelial cells and that absence of this regulation may foster ENaC hyperactivity in CF airway epithelia.

摘要

上皮钠通道（ENaC）的功能表达在囊性纤维化（CF）气道上皮中似乎升高，但发生这种情况的机制尚不清楚。我们检验了这样一个假设，即囊性纤维化跨膜电导调节因子（CFTR）改变了内源性表达的人 ENaC 在 CFBE41o-⁻ CF 支气管上皮模型中的运输。在 Ussing 室中，用阿米洛利抑制的短路电流（Isc）定义的 ENaC 的功能表达在对照条件下不存在，但在用 1 μM 地塞米松（Dex）处理 24 小时后，CFBE41o-⁻亲本和过表达 ΔF508-CFTR 的细胞中存在。Dex 的作用被糖皮质激素氢化可的松孵育模拟，但不被盐皮质激素醛固酮模拟。用胰蛋白酶处理顶端表面以激活未切割的“近沉默”ENaC，可使 Dex 处理的细胞中阿米洛利敏感的 Isc 进一步增加，而在对照细胞中无作用，表明 Dex 增加了 ENaC 细胞表面表达。相比之下，Dex 处理不会刺激 CFBE41o-⁻ 细胞中阿米洛利敏感的 Isc，这些细胞稳定表达野生型（wt）CFTR。CFBE41o-⁻wt 细胞与亲本和过表达 ΔF508-CFTR 的细胞相比，α-和 γ-ENaC 的表达也减少。此外，用胰蛋白酶处理 Dex 处理的 CFBE41o-⁻wt 细胞的顶端表面，不会刺激阿米洛利敏感的 Isc，表明即使在 Dex 处理后，ENaC 仍未出现在这些细胞的表面。我们还测试了校正转运的 ΔF508-CFTR 对 ENaC 功能表达的影响。用 1 mM 4-苯基丁酸孵育协同增加了过表达 ΔF508-CFTR 的细胞中 Dex 诱导的 ENaC 功能表达。这些数据支持这样一个假设，即 wt CFTR 可以调节气道上皮细胞中内源性 ENaC 的全细胞、功能性和表面表达，而这种调节的缺失可能促进 CF 气道上皮中 ENaC 的过度活跃。

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