Hypotonicity stimulates renal epithelial sodium transport by activating JNK via receptor tyrosine kinases.

Taruno A; Niisato N; Marunaka Y

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Hypotonicity stimulates renal epithelial sodium transport by activating JNK via receptor tyrosine kinases.

机译：低渗性通过受体酪氨酸激酶激活JNK刺激肾上皮钠运输。

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We previously reported that hypotonic stress stimulated transepithelial Na(+) transport via a pathway dependent on protein tyrosine kinase (PTK; Niisato N, Van Driessche W, Liu M, Marunaka Y. J Membr Biol 175: 63-77, 2000). However, it is still unknown what type of PTK mediates this stimulation. In the present study, we investigated the role of receptor tyrosine kinase (RTK) in the hypotonic stimulation of Na(+) transport. In renal epithelial A6 cells, we observed inhibitory effects of AG1478 [an inhibitor of the EGF receptor (EGFR)] and AG1296 [an inhibitor of the PDGF receptor (PDGFR)] on both the hypotonic stress-induced stimulation of Na(+) transport and the hypotonic stress-induced ligand-independent activation of EGFR. We further studied whether hypotonic stress activates members of the MAP kinase family, ERK1/2, p38 MAPK, and JNK/SAPK, via an RTK-dependent pathway. The present study indicates that hypotonic stress induced phosphorylation of ERK1/2 and JNK/SAPK, but not p38 MAPK, that the hypotonic stress-induced phosphorylation of ERK1/2 and JNK/SAPK was diminished by coapplication of AG1478 and AG1296, and that only JNK/SAPK was involved in the hypotonic stimulation of Na(+) transport. A further study using cyclohexamide (a protein synthesis inhibitor) suggests that both RTK and JNK/SAPK contributed to the protein synthesis-independent early phase in hypotonic stress-induced Na(+) transport, but not to the protein synthesis-dependent late phase. The present study also suggests involvement of phosphatidylinositol 3-kinase (PI3-kinase) in RTK-JNK/SAPK cascade-mediated Na(+) transport. These observations indicate that 1) hypotonic stress activates JNK/SAPK via RTKs in a ligand-independent pathway, 2) the RTK-JNK/SAPK cascade acts as a mediator of hypotonic stress for stimulation of Na(+) transport, and 3) PI3-kinase is involved in the RTK-JNK/SAPK cascade for the hypotonic stress-induced stimulation of Na(+) transport.

机译：我们先前曾报道过低渗应激通过依赖蛋白酪氨酸激酶的途径刺激跨上皮Na（+）转运（PTK; Niisato N，Van Driessche W，Liu M，Marunaka Y.J Membr Biol 175：63-77，2000）。然而，仍然不清楚哪种类型的PTK介导这种刺激。在本研究中，我们调查了受体酪氨酸激酶（RTK）在低渗Na（+）转运的刺激中的作用。在肾上皮A6细胞中，我们观察到AG1478 [EGF受体（EGFR）的抑制剂]和AG1296 [PDGF受体（PDGFR）的抑制剂]对低渗应激诱导的Na（+）转运的抑制作用和低渗应激诱导的EGFR配体非依赖性激活。我们进一步研究了低渗应激是否通过RTK依赖性途径激活MAP激酶家族，ERK1 / 2，p38 MAPK和JNK / SAPK的成员。本研究表明，低渗应激诱导的ERK1 / 2和JNK / SAPK的磷酸化，而不是p38 MAPK，低渗应激诱导的ERK1 / 2和JNK / SAPK的磷酸化被AG1478和AG1296的共同应用所减弱。 JNK / SAPK参与了Na（+）转运的低渗刺激。使用环己酰胺（一种蛋白质合成抑制剂）的进一步研究表明，RTK和JNK / SAPK都有助于低渗应激诱导的Na（+）转运过程中的蛋白质合成非依赖性早期阶段，但对蛋白质合成依赖性的非晚期阶段没有贡献。本研究还表明磷脂酰肌醇3-激酶（PI3-激酶）参与RTK-JNK / SAPK级联介导的Na（+）转运。这些观察结果表明：1）低渗应激通过配体非依赖性途径中的RTK激活JNK / SAPK，2）RTK-JNK / SAPK级联反应充当低渗应激的介质，刺激Na（+）转运，以及3）PI3 -激酶参与RTK-JNK / SAPK级联，用于低渗应激诱导的Na（+）转运刺激。

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《American Journal of Physiology》 |2007年第1期|共11页
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Taruno A; Niisato N; Marunaka Y;
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1-Phosphatidylinositol 3-Kinase; Animals; Biological Transport; Active; Blotting; Western; 1-磷脂酰肌醇3-激酶; 动物; 生物转运; 主动; 印迹法; 蛋白质; 细胞; 培养的; 酶激活;

机译：1-Phosphatidylinositol 3-Kinase;Animals;Biological Transport;Active;Blotting;Western;1-磷脂酰肌醇3-激酶;动物;生物转运;主动;印迹法;蛋白质;细胞;培养的;酶激活;

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专利

1. Hypotonicity stimulates renal epithelial sodium transport by activating JNK via receptor tyrosine kinases. [J] . Taruno A, Niisato N, Marunaka Y American Journal of Physiology . 2007,第1期

机译：低渗性通过受体酪氨酸激酶激活JNK刺激肾上皮钠运输。
2. Action of Protein Tyrosine Kinase Inhibitors on the Hypotonicity-Stimulated Trafficking Kinetics of Epithelial Na+ Channels (ENaC) in Renal Epithelial Cells: Analysis Using a Mathematical Model [J] . Marunaka R., Taruno A., Yamamoto T., Cellular Physiology and Biochemistry . 2018,第1期

机译：蛋白酪氨酸激酶抑制剂对肾上皮细胞低渗刺激的上皮Na +通道（ENaC）的运输动力学的作用：使用数学模型的分析。
3. Dopamine D2 receptor stimulation of mitogen-activated protein kinases mediated by cell type-dependent transactivation of receptor tyrosine kinases. [J] . Wang C, Buck DC, Yang R, Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry . 2005,第4期

机译：多巴胺D2受体刺激受体酪氨酸激酶的细胞类型依赖性反式激活介导的促分裂原活化蛋白激酶。
4. KG-135 Inhibits COX-2 Expression by Blocking the Activation of JNK and AP-1 in Phorbol Ester-Stimulated Human Breast Epithelial Cells [C] . SIN-AYE PARK, EUN-HEE KIM, HYE-KYUNG NA, Meeting on Cell Signaling World: Signal Transduction Pathways as Therapeutic Targets . 2007

机译：KG-135通过阻断由佛波酯刺激的人乳腺癌上皮细胞中的JNK和AP-1的活化来抑制COX-2的表达
5. Selective and specific activation of Rab5 during endocytosis of receptor tyrosine kinases. [D] . Jozic, Ivan. 2013

机译：在受体酪氨酸激酶的内吞过程中Rab5的选择性和特异性活化。
6. Hypotonicity Stimulates Potassium Flux through the WNK-SPAK/OSR1 Kinase Cascade and the Ncc69 Sodium-Potassium-2-Chloride Cotransporter in the Drosophila Renal Tubule [O] . Yipin Wu, Jeffrey N. Schellinger, Chou-Long Huang, 2014

机译：低渗性通过果蝇肾小管中的WNK-SPAK / OSR1激酶级联反应和Ncc69钾-2-氯共转运蛋白刺激钾通量。
7. Tyrosine 763 of the murine granulocyte colony-stimulating factor receptor mediates Ras-dependent activation of the JNK/SAPK mitogen-activated protein kinase pathway. [O] . Rausch, O, Marshall, C J 1997

机译：鼠粒细胞集落刺激因子受体的酪氨酸763介导JNK / SAPK丝裂原激活的蛋白激酶途径的Ras依赖性激活。
8. Increases in Tyrosine Phosphorylation Are Detectable Before Phospholipase C Activation after T Cell Receptor Stimulation. [R] . June, C. H., Fletcher, M. C., Ledbetter, J. A., 1990

机译：在T细胞受体刺激后，磷脂酶C激活前可检测到酪氨酸磷酸化的增加。

Hypotonicity stimulates renal epithelial sodium transport by activating JNK via receptor tyrosine kinases.

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