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Label-free cell phenotypic profiling decodes the composition and signaling of an endogenous ATP-sensitive potassium channel

机译：无标记细胞表型分析可解码内源性ATP敏感钾通道的组成和信号转导

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摘要

Current technologies for studying ion channels are fundamentally limited because of their inability to functionally link ion channel activity to cellular pathways. Herein, we report the use of label-free cell phenotypic profiling to decode the composition and signaling of an endogenous ATP-sensitive potassium ion channel (KATP) in HepG2C3A, a hepatocellular carcinoma cell line. Label-free cell phenotypic agonist profiling showed that pinacidil triggered characteristically similar dynamic mass redistribution (DMR) signals in A431, A549, HT29 and HepG2C3A, but not in HepG2 cells. Reverse transcriptase PCR, RNAi knockdown, and KATP blocker profiling showed that the pinacidil DMR is due to the activation of SUR2/Kir6.2 KATP channels in HepG2C3A cells. Kinase inhibition and RNAi knockdown showed that the pinacidil activated KATP channels trigger signaling through Rho kinase and Janus kinase-3, and cause actin remodeling. The results are the first demonstration of a label-free methodology to characterize the composition and signaling of an endogenous ATP-sensitive potassium ion channel.

机译：由于无法将离子通道活性与细胞途径功能性连接，目前用于研究离子通道的技术受到了根本的限制。在这里，我们报告使用无标记的细胞表型分析来解码肝细胞癌细胞HepG2C3A中内源性ATP敏感性钾离子通道（KATP）的组成和信号。无标记细胞表型激动剂分析显示，吡那地尔在A431，A549，HT29和HepG2C3A中触发特征相似的动态质量再分布（DMR）信号，但在HepG2细胞中未触发。逆转录酶PCR，RNAi敲低和KATP阻滞剂分析表明，吡那地尔DMR是由于HepG2C3A细胞中SUR2 / Kir6.2 KATP通道的激活所致。激酶抑制和RNAi抑制显示，吡那地尔活化的KATP通道通过Rho激酶和Janus激酶3触发信号传导，并导致肌动蛋白重塑。结果首次证明了无标记方法可表征内源性ATP敏感钾离子通道的组成和信号传导。

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期刊名称 Scientific Reports
作者
Haiyan Sun; Ying Wei; Huayun Deng; Qiaojie Xiong; Min Li; Joydeep Lahiri; Ye Fang;
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年(卷),期 -1(4),-1
年度 -1
页码 4934
总页数 11
原文格式 PDF
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入库时间 2022-08-21 10:58:40

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专利

1. Label-free cell phenotypic profiling decodes the composition and signaling of an endogenous ATP-sensitive potassium channel [J] . Haiyan Sun, Ying Wei, Huayun Deng, Scientific reports. . 2014,第1期

机译：无标记细胞表型分析可解码内源性ATP敏感钾通道的组成和信号转导
2. Label-free cell phenotypic profiling decodes the composition and signaling of an endogenous ATP-sensitive potassium channel [J] . Haiyan Sun, Ying Wei, Huayun Deng, Scientific reports. . 2014,第1期

机译：无标记细胞表型分析可解码内源性ATP敏感钾通道的组成和信号转导
3. Evidence for glucagon-like peptide-1 receptor signaling to activate ATP-sensitive potassium channels in pancreatic beta cells [J] . Kwon Hye-Jung, Park Hyun-Sun, Park Sung-Hee, Biochemical and Biophysical Research Communications . 2016,第2期

机译：胰高血糖素肽-1受体信号传导在胰腺β细胞中激活ATP敏感钾通道的证据
4. Role of the ATP-sensitive potassium current in extracellular potassium accumulation during myocardial ischemia: a simulation study [C] . Rodriguez, B., Ferrero, . 1998

机译：ATP敏感性钾电流在心肌缺血期间细胞外钾积累中的作用：模拟研究
5. Regulation of ATP-sensitive potassium channels in the heart. [D] . Garg, Vivek. 2009

机译：心脏中ATP敏感钾通道的调节。
6. Intracellular signalling mechanism responsible for modulation of sarcolemmal ATP-sensitive potassium channels by nitric oxide in ventricular cardiomyocytes [O] . Dai-Min Zhang, Yongping Chai, Jeffrey R Erickson, 2014

机译：一氧化氮调节心室心肌细胞对肌膜ATP敏感钾通道的调控的细胞内信号传导机制
7. Activation of ATP-sensitive potassium channels in rat pancreatic β-cells by linoleic acid through both intracellular metabolites and membrane receptor signalling pathway [O] . Yu-Feng Zhao, Jianming Pei, Chen Chen 2008

机译：亚油酸通过细胞内代谢物和膜受体信号通路通过亚油酸在大鼠胰腺β细胞中的ATP敏感钾通道的激活

Label-free cell phenotypic profiling decodes the composition and signaling of an endogenous ATP-sensitive potassium channel

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