Angiotensin III Activates Nuclear Transcription Factor-kappaB in Cultured Mesangial Cells Mainly via AT(2) Receptors: Studies with AT(1) Receptor-Knockout Mice.

Lorenzo O; Ruiz Ortega M; Suzuki Y; Ruperez M; Esteban V; Sugaya T; Egido J

首页> 外文期刊>Journal of the American Society of Nephrology: JASN >Angiotensin III Activates Nuclear Transcription Factor-kappaB in Cultured Mesangial Cells Mainly via AT(2) Receptors: Studies with AT(1) Receptor-Knockout Mice.

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Angiotensin III Activates Nuclear Transcription Factor-kappaB in Cultured Mesangial Cells Mainly via AT(2) Receptors: Studies with AT(1) Receptor-Knockout Mice.

机译：血管紧张素III主要通过AT（2）受体激活培养的系膜细胞中的核转录因子kappaB：用AT（1）受体敲除小鼠的研究。

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ABSTRACT. Nuclear factor-kappaB (NF-kappaB) regulates many genes involved in renal pathophysiologic processes. It was previously demonstrated that angiotensin II (AngII) and its amino-terminal degradation product AngIII activate NF-kappaB in mesangial cells. However, which are the Ang receptor subtypes involved in the NF-kappaB pathway and whether these Ang peptides act through the same or different receptors in mesangial cells have not been evaluated. Under the culture conditions used, quiescent rat mesangial cells expressed both AT(1) and AT(2) receptors. To investigate the receptors involved in the NF-kappaB pathway, two different approaches were used, i.e., pharmacologic studies, using specific AT(1) and AT(2) receptor antagonists and agonists, and studies in AT(1) receptor-knockout mice. In cultured rat mesangial cells, both AT(1) and AT(2) receptor antagonists inhibited AngII-induced NF-kappaB DNA binding activity, whereas NF-kappaB activation elicited by AngIII was mainly blocked by the AT(2) receptor antagonist. Similar results were observed for cytosolic IkappaBalpha degradation. An AT(2) receptor agonist also activated NF-kappaB. In AT(1) receptor-knockout murine mesangial cells, AngIII and AngII increased NF-kappaB activity and degraded cytosolic IkappaBalpha; both processes were blocked by the AT(2) receptor antagonist. These data demonstrate that, in mesangial cells, NF-kappaB activation is mediated by AT(1) and AT(2) receptors, suggesting a novel intracellular signaling mechanism for AT(2) receptors in the kidney. Some differences in Ang peptide receptor-mediated responses were also observed. AngII activates NF-kappaB via AT(1) and AT(2) receptors, whereas AngIII acts mainly via AT(2) receptors. These results suggest the potential involvement of the AngIII/AT(2) receptor/NF-kappaB pathway in pathophysiologic processes in the kidney and provide a better understanding of the renin-angiotensin system.

机译：抽象。核因子-κB（NF-kappaB）调节与肾脏病理生理过程有关的许多基因。先前已证明血管紧张素II（AngII）及其氨基末端降解产物AngIII激活肾小球膜细胞中的NF-κB。然而，尚未评估涉及NF-κB途径的Ang受体亚型以及这些Ang肽是否通过肾小球膜细胞中的相同或不同受体起作用。在使用的培养条件下，静止的大鼠肾小球系膜细胞同时表达AT（1）和AT（2）受体。为了研究参与NF-kappaB途径的受体，使用了两种不同的方法，即药理研究，使用特定的AT（1）和AT（2）受体拮抗剂和激动剂，以及在AT（1）受体敲除小鼠中的研究。在培养的大鼠系膜细胞中，AT（1）和AT（2）受体拮抗剂均抑制AngII诱导的NF-kappaB DNA结合活性，而AngIII引起的NF-kappaB激活主要被AT（2）受体拮抗剂阻断。对于胞质IkappaBalpha降解观察到相似的结果。 AT（2）受体激动剂也激活了NF-κB。在AT（1）受体敲除小鼠系膜细胞中，AngIII和AngII增加了NF-kappaB的活性并降解了胞浆IkappaBalpha。这两个过程均被AT（2）受体拮抗剂阻断。这些数据表明，在肾小球系膜细胞中，NF-κB激活是由AT（1）和AT（2）受体介导的，提示肾脏中AT（2）受体的新型细胞内信号传导机制。还观察到Ang肽受体介导的反应中的一些差异。 AngII通过AT（1）和AT（2）受体激活NF-κB，而AngIII主要通过AT（2）受体起作用。这些结果表明，AngIII / AT（2）受体/NF-κB通路可能参与了肾脏的病理生理过程，并提供了对肾素-血管紧张素系统的更好理解。

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来源
《Journal of the American Society of Nephrology: JASN》 |2002年第5期|共10页
作者
Lorenzo O; Ruiz Ortega M; Suzuki Y; Ruperez M; Esteban V; Sugaya T; Egido J;
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正文语种 eng
中图分类泌尿科学（泌尿生殖系疾病）;
关键词
Not free of; angiotensin II type 2 receptor; Mesangial cell;

机译：不无;血管紧张素Ⅱ2型受体;肾小球膜细胞;

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1. Angiotensin III Activates Nuclear Transcription Factor-kappaB in Cultured Mesangial Cells Mainly via AT(2) Receptors: Studies with AT(1) Receptor-Knockout Mice. [J] . Lorenzo O, Ruiz Ortega M, Suzuki Y, Journal of the American Society of Nephrology: JASN . 2002,第5期

机译：血管紧张素III主要通过AT（2）受体激活培养的系膜细胞中的核转录因子kappaB：用AT（1）受体敲除小鼠的研究。
2. Angiotensin III increases MCP-1 and activates NF-|[kgr]|B and AP-1 in cultured mesangial and mononuclear cells [J] . Marta Ruiz-Ortega, Oscar Lorenzo, Jesus Egido Kidney international. . 2000,第6期

机译：血管紧张素III增加了培养的肾小球系膜和单核细胞中的MCP-1并激活NF- | [kgr] | B和AP-1
3. Angiotensin II, via angiotensin receptor type 1uclear factor-κB activation, causes a synergistic effect on interleukin-1-β-induced inflammatory responses in cultured mesangial cells [J] . Matilde Alique, Elsa Sánchez-López, Sandra Rayego-Mateos, Journal of Renin-Angiotensin-Aldosterone System . 2015,第1期

机译：血管紧张素II通过1型血管紧张素受体/核因子-κB的活化，对白介素-1-β诱导的系膜细胞炎症反应产生协同作用
4. Transcriptional Regulatory Mechanismsof the Human ApoA-I/ApoCIII GeneCluster in vitro and in Trangenic Mice:The Role of Nuclear Receptors [C] . World Association for Laser Therapy . 2002

机译：体外和长核小鼠的人apoa-i / apociii genecluster的转录调节机制：核受体的作用
5. Disulfide bond formation in the nuclear factor-kappaB essential modulator and gene expression profiling of a human B-lymphoma cell line expressing an activated REL transcription factor. [D] . Herscovitch, Melanie I. 2010

机译：核因子-κB必需调节剂中的二硫键形成和表达激活的REL转录因子的人B淋巴瘤细胞系的基因表达谱。
6. Intracellular angiotensin II directly induces in vitro transcription of TGF-β1 MCP-1 and NHE-3 mRNAs in isolated rat renal cortical nuclei via activation of nuclear AT1 receptors [O] . Xiao C. Li, Jia L. Zhuo -1

机译：细胞内血管紧张素II通过激活核AT1受体直接诱导离体大鼠肾皮质核中TGF-β1MCP-1和NHE-3 mRNA的体外转录
7. Angiotensin III Activates Nuclear Transcription Factor-κB in Cultured Mesangial Cells Mainly via AT2Receptors: Studies with AT1Receptor-Knockout Mice [O] . Óscar Lorenzo, Marta Ruiz-Ortega, Yusuke Suzuki, 2002

机译：血管紧张素III主要通过AT2RECEPTORS激活培养的膜神经细胞中的核转录因子-κB：用AT1receptor-Nockout小鼠研究

Angiotensin III Activates Nuclear Transcription Factor-kappaB in Cultured Mesangial Cells Mainly via AT(2) Receptors: Studies with AT(1) Receptor-Knockout Mice.

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