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PKA 和 PIAS3 之间的串扰调节心脏 Kv4 通道 SUMOylation。

Crosstalk between PKA and PIAS3 regulates cardiac Kv4 channel SUMOylation.

机构信息

Department of Biology, Georgia State University, Atlanta, GA, USA.

Present Address: Section on Molecular Neurophysiology and Biophysics, Eunice Kennedy Shriver National Institute of Child Health and Human Development, Bethesda, MD, USA.

出版信息

Cell Commun Signal. 2024 Sep 2;22(1):422. doi: 10.1186/s12964-024-01795-4.

DOI:10.1186/s12964-024-01795-4
PMID:39223673
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11367828/
Abstract

Post-translational SUMOylation of nuclear and cytosolic proteins maintains homeostasis in eukaryotic cells and orchestrates programmed responses to changes in metabolic demand or extracellular stimuli. In excitable cells, SUMOylation tunes the biophysical properties and trafficking of ion channels. Ion channel SUMOylation status is determined by the opposing enzyme activities of SUMO ligases and deconjugases. Phosphorylation also plays a permissive role in SUMOylation. SUMO deconjugases have been identified for several ion channels, but their corresponding E3 ligases remain unknown. This study shows PIAS3, a.k.a. KChAP, is a bona fide SUMO E3 ligase for Kv4.2 and HCN2 channels in HEK cells, and endogenous Kv4.2 and Kv4.3 channels in cardiomyocytes. PIAS3-mediated SUMOylation at Kv4.2-K579 increases channel surface expression through a rab11a-dependent recycling mechanism. PKA phosphorylation at Kv4.2-S552 reduces the current mediated by Kv4 channels in HEK293 cells, cardiomyocytes, and neurons. This study shows PKA mediated phosphorylation blocks Kv4.2-K579 SUMOylation in HEK cells and cardiomyocytes. Together, these data identify PIAS3 as a key downstream mediator in signaling cascades that control ion channel surface expression.

摘要

蛋白质翻译后 SUMO 化修饰作用于核蛋白和胞浆蛋白,维持真核细胞内的稳态平衡,并协调细胞对代谢需求或细胞外刺激变化的程序化响应。在可兴奋细胞中,SUMO 化修饰作用于离子通道的生物物理特性和运输过程。离子通道 SUMO 化状态由 SUMO 连接酶和去 SUMO 酶的相反酶活性决定。磷酸化也在 SUMO 化中起许可作用。已经鉴定出几种离子通道的 SUMO 去 SUMO 酶,但它们相应的 E3 连接酶仍然未知。本研究表明,PIAS3(又名 KChAP)是 HEK 细胞中 Kv4.2 和 HCN2 通道以及心肌细胞中内源性 Kv4.2 和 Kv4.3 通道的真正 SUMO E3 连接酶。PIAS3 介导的 Kv4.2-K579 的 SUMO 化通过 rab11a 依赖的回收机制增加了通道的表面表达。Kv4.2-S552 处 PKA 的磷酸化降低了 HEK293 细胞、心肌细胞和神经元中 Kv4 通道介导的电流。本研究表明,PKA 介导的磷酸化阻止了 HEK 细胞和心肌细胞中 Kv4.2-K579 的 SUMO 化。总之,这些数据表明,PIAS3 是控制离子通道表面表达的信号级联中的关键下游介质。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/84ae/11367828/7b5f762fccb0/12964_2024_1795_Fig1_HTML.jpg

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