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Targeted disruption of the heat shock protein 20–phosphodiesterase 4D (PDE4D) interaction protects against pathological cardiac remodelling in a mouse model of hypertrophy

机译：有针对性地破坏热休克蛋白20-磷酸二酯酶4D（PDE4D）相互作用可防止肥大的小鼠模型发生病理性心脏重塑

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摘要

Phosphorylated heat shock protein 20 (HSP20) is cardioprotective. Using human induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs) and a mouse model of pressure overload mediated hypertrophy, we show that peptide disruption of the HSP20–phosphodiesterase 4D (PDE4D) complex results in attenuation of action potential prolongation and protection against adverse cardiac remodelling. The later was evidenced by improved contractility, decreased heart weight to body weight ratio, and reduced interstitial and perivascular fibrosis. This study demonstrates that disruption of the specific HSP20–PDE4D interaction leads to attenuation of pathological cardiac remodelling.

机译：磷酸化的热休克蛋白20（HSP20）具有心脏保护作用。使用人类诱导的多能干细胞衍生的心肌细胞（hiPSC-CMs）和压力超负荷介导的肥大的小鼠模型，我们显示HSP20-磷酸二酯酶4D（PDE4D）复合物的肽破坏导致动作电位延长的减弱和对不良反应的保护心脏重塑。后者通过改善收缩力，降低心脏重量与体重比以及减少组织间和血管周围纤维化来证明。这项研究表明，特定的HSP20-PDE4D相互作用的破坏导致病理性心脏重塑的减弱。

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期刊名称 Wiley-Blackwell Online Open
作者
Tamara P. Martin; Maria P. Hortigon-Vinagre; Jane E. Findlay; Christina Elliott; Susan Currie; George S. Baillie;
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作者单位

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年(卷),期 -1(4),-1
年度 -1
页码 923–927
总页数 5
原文格式 PDF
正文语种
中图分类
关键词
cAMP PDE4D HSP20 Cardiac remodeling Cardiac hypertrophy Peptide disruption;

机译：cAMP;PDE4D;HSP20;心脏重塑;心脏肥大;肽破坏;

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外文文献

1. Targeted disruption of the heat shock protein 20-phosphodiesterase 4D (PDE4D) interaction protects against pathological cardiac remodelling in a mouse model of hypertrophy [J] . Tamara P. Martin, Maria P. Hortigon-Vinagre, Jane E. Findlay, FEBS Open Bio . 2014,第4期

机译：有针对性地破坏热休克蛋白20-磷酸二酯酶4D（PDE4D）相互作用可以防止肥大的小鼠模型中的病理性心脏重塑
2. Therapeutic Cardiac-Targeted Delivery of miR-1 Reverses Pressure Overload–Induced Cardiac Hypertrophy and Attenuates Pathological Remodeling [J] . Antoine H. Chaanine, Bertrand N. Mukete, Djamel Lebeche, Journal of the American Heart Association Cardiovascular and Cerebrovascular Disease . 2013,第3期

机译：以治疗为目标的miR-1心脏传递可以逆转压力超负荷引起的心脏肥大并减轻病理重塑
3. H-1 NMR structural and functional characterisation of a cAMP-specific phosphodiesterase-4D5 (PDE4D5) N-terminal region peptide that disrupts PDE4D5 interaction with the signalling scaffold proteins, arrestin and RACK1 [J] . Smith KJ, Baillie GS, Hyde EI, Cellular Signalling . 2007,第12期

机译：H-1 NMR的cAMP特异性磷酸二酯酶4D5（PDE4D5）N端区域肽的结构和功能表征，可破坏PDE4D5与信号支架蛋白，抑制蛋白和RACK1的相互作用
4. The role of small heat shock protein 20 and its phosphorylation in the regulation of cardiac function and ischemia/reperfusion injury [D] . Qian, Jiang 2010

机译：小型热休克蛋白20及其磷酸化在调节心脏功能和缺血/再灌注损伤中的作用
5. Multiple Behavior Phenotypes of the Fragile-X Syndrome Mouse Model Respond to Chronic Inhibition of Phosphodiesterase-4D (PDE4D) [O] . Mark E. Gurney, Patricia Cogram, Robert M Deacon, -1

机译：易碎X综合征小鼠模型的多种行为表型对磷酸二酯酶4D（PDE4D）的慢性抑制作出反应。
6. Targeted disruption of the heat shock protein 20–phosphodiesterase 4D (PDE4D) interaction protects against pathological cardiac remodelling in a mouse model of hypertrophy [O] . Martin, Tamara, Hortigon-Vinagre, Maria, Findlay, Jane, 2014

机译：有针对性地破坏热休克蛋白20-磷酸二酯酶4D（PDE4D）相互作用可以防止肥大的小鼠模型发生病理性心脏重塑

Targeted disruption of the heat shock protein 20–phosphodiesterase 4D (PDE4D) interaction protects against pathological cardiac remodelling in a mouse model of hypertrophy

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