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表皮生长因子(EGF)和前列腺素E2(PGE2)对兔近端肾小管基底外侧有机阴离子摄取及人肾上皮细胞中表达的人有机阴离子转运体1(hOAT1)的作用。

Action of EGF and PGE2 on basolateral organic anion uptake in rabbit proximal renal tubules and hOAT1 expressed in human kidney epithelial cells.

作者信息

Sauvant C, Hesse D, Holzinger H, Evans K K, Dantzler W H, Gekle M

机构信息

Physiologisches Institut, Universität Würzburg, Röntgenring 9, 97070 Würzburg, Germany.

出版信息

Am J Physiol Renal Physiol. 2004 Apr;286(4):F774-83. doi: 10.1152/ajprenal.00326.2003. Epub 2003 Nov 25.

Abstract

We recently showed that, in a proximal tubule cell line (opossum kidney cells), epithelial growth factor (EGF) stimulates basolateral organic anion transport (OAT) via ERK1/2, arachidonic acid, phospholipase A2, and generation of prostaglandins. PGE2 binds the prostanoid receptor and, thus, activates adenylate cyclase and PKA, which stimulate basolateral organic anion uptake. In the present study, we investigated whether this regulatory cascade is also true 1) for ex vivo conditions in isolated renal proximal (S2) tubules from rabbit and 2) in a human renal epithelial cell line stably expressing human OAT1 (IHKE-hOAT1). EGF activated ERK1/2 in S2 tubules and IHKE-hOAT1, and, in both cases, inhibition of ERK activation (by U-0126) abolished this stimulation. In S2 tubules and IHKE-hOAT1, EGF led to an increase of organic anion uptake, which again was inhibited by U-0126. PGE2 stimulated basolateral organic anion uptake in rabbit S2 tubules and IHKE-hOAT1. EGF- and PGE2-mediated stimulation of organic anion uptake was abolished by inhibition of PKA in rabbit S2 tubules and IHKE-hOAT1, respectively. We conclude that 1) stimulation of basolateral organic anion uptake by EGF or PGE2 is a widespread (if not general) regulatory mechanism, 2) the signal transduction pathway involved seems to be general, 3) stimulation of basolateral organic anion uptake by EGF or PGE2 is also present under ex vivo conditions and, thus, is not a cell culture artifact, 4) activation of OAT1 is sufficient to explain the stimulatory effects of EGF and PGE2 in opossum kidney cells and rabbit S2 segments, and 5) stimulation of basolateral OAT1 by EGF or PGE2 is also important in humans and, thus, may have clinical implications.

摘要

我们最近发现,在近端肾小管细胞系(负鼠肾细胞)中,表皮生长因子(EGF)通过细胞外调节蛋白激酶1/2(ERK1/2)、花生四烯酸、磷脂酶A2以及前列腺素的生成来刺激基底外侧有机阴离子转运(OAT)。前列腺素E2(PGE2)与前列腺素受体结合,从而激活腺苷酸环化酶和蛋白激酶A(PKA),进而刺激基底外侧有机阴离子摄取。在本研究中,我们调查了这种调节级联反应是否也适用于以下两种情况:1)兔离体肾近端(S2)小管的体外条件;2)稳定表达人OAT1的人肾上皮细胞系(IHKE-hOAT1)。EGF在S2小管和IHKE-hOAT1中激活了ERK1/2,并且在这两种情况下,抑制ERK激活(通过U-0126)都消除了这种刺激作用。在S2小管和IHKE-hOAT1中,EGF导致有机阴离子摄取增加,而这再次被U-0126抑制。PGE2刺激兔S2小管和IHKE-hOAT1中的基底外侧有机阴离子摄取。分别在兔S2小管和IHKE-hOAT1中,通过抑制PKA消除了EGF和PGE2介导的有机阴离子摄取刺激。我们得出以下结论:1)EGF或PGE2对基底外侧有机阴离子摄取的刺激是一种广泛存在(即便不是普遍存在)的调节机制;2)所涉及的信号转导途径似乎是普遍的;3)EGF或PGE2对基底外侧有机阴离子摄取的刺激在体外条件下也存在,因此并非细胞培养假象;4)OAT1的激活足以解释EGF和PGE2在负鼠肾细胞和兔S2节段中的刺激作用;5)EGF或PGE2对基底外侧OAT1的刺激在人类中也很重要,因此可能具有临床意义。

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