Thomas Christie P, Campbell Jason R, Wright Patrick J, Husted Russell F
Department of Internal Medicine, University of Iowa College of Medicine, Iowa City, Iowa 52242, USA.
Am J Physiol Lung Cell Mol Physiol. 2004 Oct;287(4):L843-51. doi: 10.1152/ajplung.00340.2003. Epub 2004 Jun 18.
H441 cells, a bronchiolar epithelial cell line, develop a cAMP-regulated benzamil-sensitive Na+ transport pathway on permeable supports (Itani OA, Auerbach SD, Husted RF, Volk KA, Ageloff S, Knepper MA, Stokes JB, Thomas CP. Am J Physiol Lung Cell Mol Physiol 282: L631-L641, 2002). To understand the molecular basis for the stimulation of Na+ transport, we delineated the role of specific intracellular pathways and examined the effect of cAMP on alphabetagamma-epithelial Na+ channel (ENaC) and sgk1 expression. Na+ transport increases within 5 min of cAMP stimulation and is sustained for >24 h. The sustained effect of cAMP on Na+ transport is abolished by LY-294002, an inhibitor of phosphatidylinositol 3-kinase, by H89, an inhibitor of PKA, or by SB-202190, an inhibitor of p38 MAP kinase. The sustained effect of cAMP was associated with increases in alpha-ENaC mRNA and protein but without a detectable increase in betagamma-ENaC and sgk1. The early effect of cAMP on Na+ transport is brefeldin sensitive and is mediated via PKA. These results are consistent with a model where the early effect of cAMP is to increase trafficking of Na+ channels to the apical cell surface whereas the sustained effect requires the synthesis of alpha-ENaC.
H441细胞是一种细支气管上皮细胞系,在可渗透支持物上可形成一种受cAMP调节的、对苯甲酰amil敏感的Na⁺转运途径(伊塔尼·奥阿、奥尔巴赫·斯德、赫斯特德·罗夫、沃尔克·卡、阿盖洛夫·斯、克内珀·马、斯托克斯·杰布、托马斯·西普。《美国生理学杂志:肺细胞与分子生理学》282:L631 - L641,2002年)。为了解刺激Na⁺转运的分子基础,我们明确了特定细胞内途径的作用,并研究了cAMP对αβγ - 上皮钠通道(ENaC)和sgk1表达的影响。cAMP刺激后5分钟内Na⁺转运增加,并持续超过24小时。cAMP对Na⁺转运的持续作用可被磷脂酰肌醇3 - 激酶抑制剂LY - 294002、蛋白激酶A抑制剂H89或p38丝裂原活化蛋白激酶抑制剂SB - 202190消除。cAMP的持续作用与α - ENaC mRNA和蛋白增加相关,但βγ - ENaC和sgk1未检测到增加。cAMP对Na⁺转运的早期作用对布雷菲德菌素敏感,且由蛋白激酶A介导。这些结果与一个模型一致,即cAMP的早期作用是增加钠通道向细胞顶端表面的转运,而持续作用则需要α - ENaC的合成。
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