Phosphorylation of Shox2 Is Required for Its Function to Control Sinoatrial Node Formation

机译：Shox2的磷酸化是其控制窦房结形成的功能所必需的

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BackgroundInactivation of Shox2, a member of the short‐stature homeobox gene family, leads to defective development of multiple organs and embryonic lethality as a result of cardiovascular defects, including bradycardia and severe hypoplastic sinoatrial node (SAN) and sinus valves, in mice. It has been demonstrated that Shox2 regulates a genetic network through the repression of Nkx2.5 to maintain the fate of the SAN cells. However, the functional mechanism of Shox2 protein as a transcriptional repressor on Nkx2.5 expression remains completely unknown.

机译：背景矮身形同源盒基因家族成员Shox2的失活导致心血管缺陷（包括心动过缓，严重的增生性窦房结（SAN）和窦静脉瓣膜）导致多器官发育不良和胚胎致死性。已经证明，Shox2通过抑制Nkx2.5来调节遗传网络，以维持SAN细胞的命运。但是，Shox2蛋白作为转录阻遏物对Nkx2.5表达的功能机制仍然完全未知。

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期刊名称 Journal of the American Heart Association: Cardiovascular and Cerebrovascular Disease
作者
Hongbing Liu; Chao‐Hui Chen; Wenduo Ye; Ramón A. Espinoza‐Lewis; Xuefeng Hu; Yanding Zhang; YiPing Chen;
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作者单位

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年(卷),期 2014(3),3
年度 2014
页码 e000796
总页数 14
原文格式 PDF
正文语种
中图分类心血管疾病;
关键词
DNA binding Nkx2.5 repression pacemaking phosphorylation SAN development Shox2;

机译：DNA结合;Nkx2.5抑制;起搏;磷酸化;SAN开发;Shox2;

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专利

1. Functional Redundancy between Human SHOX and Mouse Shox2 Genes in the Regulation of Sinoatrial Node Formation and Pacemaking Function [J] . Hongbing Liu, Chao-Hui Chen, Ramón Espinoza-Lewis, The Journal of biological chemistry . 2011,第19期

机译：窦房结节点形成和起重术函数中人沉和小鼠Shox2基因的功能冗余
2. Sophisticated architecture is required for the sinoatrial node to perform its normal pacemaker function. [J] . Boyett MR, Dobrzynski H, Lancaster MK, Journal of cardiovascular electrophysiology . 2003,第1期

机译：窦房结需要复杂的架构来执行其正常的起搏器功能。
3. Tbx3 controls the sinoatrial node gene program and imposes pacemaker function on the atria. [J] . Hoogaars WM, Engel A, Brons JF, Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses . 2007,第9期

机译：Tbx3控制窦房结基因程序，并在心房上施加起搏器功能。
4. In Silico Screening of the Key Electrical Remodelling Targets in Atrial Fibrillation-Induced Sinoatrial Node Dysfunction [C] . Jieyun Bai, Yaosheng Lu, Roshan Sharma, Computing in Cardiology Conference . 2019

机译：房颤诱发的窦房结功能障碍关键电重构目标的计算机筛选
5. Mathematical Modeling of Sinoatrial Node Dynamics at the Subcellular, Cellular, and Tissue Scales [D] . Meyer, Emily E. 2021

机译：亚细胞，蜂窝和组织尺度窦房结动力学的数学建模
6. Functional Redundancy between Human SHOX and Mouse Shox2 Genes in the Regulation of Sinoatrial Node Formation and Pacemaking Function [O] . Hongbing Liu, Chao-Hui Chen, Ramón A. Espinoza-Lewis, 2011

机译：人SHOX和小鼠Shox2基因之间的功能冗余在窦房结形成和起搏功能的调节中。
7. Functional Redundancy between Human SHOX and Mouse Shox2 Genes in the Regulation of Sinoatrial Node Formation and Pacemaking Function* [O] . Liu, Hongbing, Chen, Chao-Hui, Espinoza-Lewis, Ramón A., 2011

机译：人SHOX和小鼠Shox2基因在窦房结形成和起搏功能调控中的功能冗余*

Phosphorylation of Shox2 Is Required for Its Function to Control Sinoatrial Node Formation

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