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肌球蛋白重链异构体在衰竭和非衰竭人类心脏中的表达。

Myosin heavy chain isoform expression in the failing and nonfailing human heart.

作者信息

Miyata S, Minobe W, Bristow M R, Leinwand L A

机构信息

Department of Molecular, Cellular and Developmental Biology, University of Colorado at Boulder, Boulder, CO 80309-0347, USA.

出版信息

Circ Res. 2000 Mar 3;86(4):386-90. doi: 10.1161/01.res.86.4.386.

Abstract

In the heart, the relative proportions of the 2 forms of the motor protein myosin heavy chain (MyHC) have been shown to be affected by a wide variety of pathological and physiological stimuli. Hearts that express the faster MyHC motor protein, alpha, produce more power than those expressing the slower MyHC motor protein, beta, leading to the hypothesis that MyHC isoforms play a major role in the determination of cardiac contractility. We showed previously that a significant amount of alphaMyHC mRNA is expressed in nonfailing human ventricular myocardium and that alphaMyHC mRNA expression is decreased 15-fold in end-stage failing left ventricles. In the present study, we determined the MyHC protein isoform content of human heart samples of known MyHC mRNA composition. We demonstrate that alphaMyHC protein was easily detectable in 12 nonfailing hearts. alphaMyHC protein represented 7.2+/-3.2% of total MyHC protein (compared with approximately 35% of the MyHC mRNA), suggesting that translational regulation may be operative; in contrast, there was effectively no detectable alphaMyHC protein in the left ventricles of 10 end-stage failing human hearts.

摘要

在心脏中,已表明运动蛋白肌球蛋白重链(MyHC)的两种形式的相对比例会受到多种病理和生理刺激的影响。表达速度更快的MyHC运动蛋白α的心脏比表达速度较慢的MyHC运动蛋白β的心脏产生更多的力量,这导致了一种假说,即MyHC同工型在心脏收缩力的决定中起主要作用。我们之前表明,大量的αMyHC mRNA在非衰竭的人类心室心肌中表达,并且在终末期衰竭的左心室中αMyHC mRNA表达降低了15倍。在本研究中,我们确定了已知MyHC mRNA组成的人类心脏样本中的MyHC蛋白同工型含量。我们证明,在12个非衰竭心脏中很容易检测到αMyHC蛋白。αMyHC蛋白占总MyHC蛋白的7.2±3.2%(相比之下,MyHC mRNA约占35%),这表明翻译调控可能起作用;相反,在10个终末期衰竭的人类心脏的左心室中实际上没有可检测到的αMyHC蛋白。

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