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来自异位表达肠道γ-肌动蛋白的小鼠心脏肌丝中的钙离子激活和张力消耗

Ca(2+) activation and tension cost in myofilaments from mouse hearts ectopically expressing enteric gamma-actin.

作者信息

Martin Anne F, Phillips Ronald M, Kumar Ajit, Crawford Kelly, Abbas Zainab, Lessard James L, de Tombe Pieter, Solaro R John

机构信息

Department of Physiology and Biophysics, M/C 901, University of Illinois at Chicago, 835 S. Wolcott Avenue, Chicago, IL 60612, USA.

出版信息

Am J Physiol Heart Circ Physiol. 2002 Aug;283(2):H642-9. doi: 10.1152/ajpheart.00890.2001.

Abstract

To determine the significance of actin isoforms in chemomechanical coupling, we compared tension and ATPase rate in heart myofilaments from nontransgenic (NTG) and transgenic (TG) mice in which enteric gamma-actin replaced >95% of the cardiac alpha-actin. Enteric gamma-actin was expressed against three backgrounds: mice expressing cardiac alpha-actin, heterozygous null cardiac alpha-actin mice, and homozygous null cardiac alpha-actin mice. There were no differences in maximum Ca(2+) activated tension or maximum rate of tension redevelopment after a quick release and rapid restretch protocol between TG and NTG skinned fiber bundles. However, compared with NTG controls, Ca(2+) sensitivity of tension was significantly decreased and economy of tension development was significantly increased in myofilaments from all TG hearts. Shifts in myosin isoform population could not fully account for this increase in the economy of force production of TG myofilaments. Our results indicate that an exchange of cardiac alpha-actin with an actin isoform differing in only five amino acids has a significant impact on both Ca(2+) regulation of cardiac myofilaments and the cross-bridge cycling rate.

摘要

为了确定肌动蛋白异构体在化学机械偶联中的重要性,我们比较了非转基因(NTG)和转基因(TG)小鼠心肌肌丝中的张力和ATP酶活性。在转基因小鼠中,肠道γ-肌动蛋白取代了>95%的心脏α-肌动蛋白。肠道γ-肌动蛋白在三种背景下表达:表达心脏α-肌动蛋白的小鼠、杂合性心脏α-肌动蛋白缺失小鼠和纯合性心脏α-肌动蛋白缺失小鼠。在快速释放和快速再拉伸实验后,TG和NTG去皮纤维束之间的最大Ca(2+)激活张力或张力再发展的最大速率没有差异。然而,与NTG对照组相比,所有TG心脏的肌丝中,张力的Ca(2+)敏感性显著降低,张力发展的经济性显著增加。肌球蛋白异构体群体的变化不能完全解释TG肌丝中力产生经济性的增加。我们的结果表明,仅五个氨基酸不同的肌动蛋白异构体与心脏α-肌动蛋白的交换对心肌肌丝的Ca(2+)调节和横桥循环速率都有显著影响。

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