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本文引用的文献

1
Genetic inhibition of cardiac ERK1/2 promotes stress-induced apoptosis and heart failure but has no effect on hypertrophy in vivo.心脏ERK1/2的基因抑制促进应激诱导的细胞凋亡和心力衰竭,但对体内肥大无影响。
Proc Natl Acad Sci U S A. 2007 Aug 28;104(35):14074-9. doi: 10.1073/pnas.0610906104. Epub 2007 Aug 20.
2
KSR and CNK: two scaffolds regulating RAS-mediated RAF activation.KSR和CNK:两种调节RAS介导的RAF激活的支架蛋白。
Oncogene. 2007 May 14;26(22):3143-58. doi: 10.1038/sj.onc.1210408.
3
Sense and stretchability: the role of titin and titin-associated proteins in myocardial stress-sensing and mechanical dysfunction.感知与伸展性:肌联蛋白及肌联蛋白相关蛋白在心肌应力感知和机械功能障碍中的作用
Cardiovasc Res. 2008 Mar 1;77(4):637-48. doi: 10.1016/j.cardiores.2007.03.029.
4
FHL3 binds MyoD and negatively regulates myotube formation.FHL3 结合 MyoD 并负向调节肌管形成。
J Cell Sci. 2007 Apr 15;120(Pt 8):1423-35. doi: 10.1242/jcs.004739. Epub 2007 Mar 27.
5
Targeted deletion of titin N2B region leads to diastolic dysfunction and cardiac atrophy.肌联蛋白N2B区域的靶向缺失导致舒张功能障碍和心脏萎缩。
Proc Natl Acad Sci U S A. 2007 Feb 27;104(9):3444-9. doi: 10.1073/pnas.0608543104. Epub 2007 Feb 20.
6
The role of scaffold proteins in MEK/ERK signalling.支架蛋白在MEK/ERK信号传导中的作用。
Biochem Soc Trans. 2006 Nov;34(Pt 5):833-6. doi: 10.1042/BST0340833.
7
alpha-E-catenin inactivation disrupts the cardiomyocyte adherens junction, resulting in cardiomyopathy and susceptibility to wall rupture.α-E-连环蛋白失活会破坏心肌细胞黏附连接,导致心肌病和易发生壁破裂。
Circulation. 2006 Sep 5;114(10):1046-55. doi: 10.1161/CIRCULATIONAHA.106.634469. Epub 2006 Aug 21.
8
Cardiac titin: structure, functions and role in disease.心肌肌联蛋白:结构、功能及在疾病中的作用
Clin Chim Acta. 2007 Jan;375(1-2):1-9. doi: 10.1016/j.cca.2006.06.035. Epub 2006 Jul 7.
9
Functional analysis of titin/connectin N2-B mutations found in cardiomyopathy.在心肌病中发现的肌联蛋白/连接蛋白N2-B突变的功能分析。
J Muscle Res Cell Motil. 2005;26(6-8):367-74. doi: 10.1007/s10974-005-9018-5.
10
The multifunctional roles of the four-and-a-half-LIM only protein FHL2.四半LIM结构域蛋白FHL2的多功能作用
Cell Mol Life Sci. 2006 Feb;63(3):268-84. doi: 10.1007/s00018-005-5438-z.

心肌细胞肌节内包含FHL1的复合物介导小鼠肥厚性生物力学应激反应。

An FHL1-containing complex within the cardiomyocyte sarcomere mediates hypertrophic biomechanical stress responses in mice.

作者信息

Sheikh Farah, Raskin Anna, Chu Pao-Hsien, Lange Stephan, Domenighetti Andrea A, Zheng Ming, Liang Xingqun, Zhang Tong, Yajima Toshitaka, Gu Yusu, Dalton Nancy D, Mahata Sushil K, Dorn Gerald W, Brown Joan Heller, Peterson Kirk L, Omens Jeffrey H, McCulloch Andrew D, Chen Ju

机构信息

Department of Medicine, UCSD, La Jolla, California 92093, USA.

出版信息

J Clin Invest. 2008 Dec;118(12):3870-80. doi: 10.1172/JCI34472. Epub 2008 Nov 3.

DOI:10.1172/JCI34472
PMID:19033658
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2575833/
Abstract

The response of cardiomyocytes to biomechanical stress can determine the pathophysiology of hypertrophic cardiac disease, and targeting the pathways regulating these responses is a therapeutic goal. However, little is known about how biomechanical stress is sensed by the cardiomyocyte sarcomere to transduce intracellular hypertrophic signals or how the dysfunction of these pathways may lead to disease. Here, we found that four-and-a-half LIM domains 1 (FHL1) is part of a complex within the cardiomyocyte sarcomere that senses the biomechanical stress-induced responses important for cardiac hypertrophy. Mice lacking Fhl1 displayed a blunted hypertrophic response and a beneficial functional response to pressure overload induced by transverse aortic constriction. A link to the Galphaq (Gq) signaling pathway was also observed, as Fhl1 deficiency prevented the cardiomyopathy observed in Gq transgenic mice. Mechanistic studies demonstrated that FHL1 plays an important role in the mechanism of pathological hypertrophy by sensing biomechanical stress responses via the N2B stretch sensor domain of titin and initiating changes in the titin- and MAPK-mediated responses important for sarcomere extensibility and intracellular signaling. These studies shed light on the physiological regulation of the sarcomere in response to hypertrophic stress.

摘要

心肌细胞对生物力学应激的反应可决定肥厚性心脏病的病理生理学,而针对调节这些反应的信号通路是一个治疗目标。然而,关于心肌细胞肌节如何感知生物力学应激以转导细胞内肥厚信号,或者这些信号通路的功能障碍如何导致疾病,我们所知甚少。在此,我们发现四又二分之一LIM结构域1(FHL1)是心肌细胞肌节内一个复合体的组成部分,该复合体可感知对心脏肥大至关重要的生物力学应激诱导反应。缺乏Fhl1的小鼠对横向主动脉缩窄诱导的压力过载表现出减弱的肥厚反应和有益的功能反应。还观察到与Gαq(Gq)信号通路的联系,因为Fhl1缺陷可预防在Gq转基因小鼠中观察到的心肌病。机制研究表明,FHL1通过肌联蛋白的N2B拉伸传感器结构域感知生物力学应激反应,并启动对肌节伸展性和细胞内信号传导重要的肌联蛋白和丝裂原活化蛋白激酶介导反应的变化,从而在病理性肥大机制中发挥重要作用。这些研究揭示了肌节对肥厚应激的生理调节机制。