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用心房轻链1重构心室肌球蛋白可改善其功能特性。

Reconstitution of ventricular myosin with atrial light chains 1 improves its functional properties.

作者信息

Khalina Yana N, Bartsch Holger, Petzhold Daria, Haase Hannelore, Podlubnaya Zoya A, Shpagina Mila D, Morano Ingo

机构信息

Institute of Theoretical and Experimental Biophysics RAS, Laboratory of Structure and Function of Muscle Proteins, Pushchino, Russia.

出版信息

Acta Biochim Pol. 2005;52(2):443-8. Epub 2005 May 15.

Abstract

Atrial light chain 1 (ALC-1) is expressed in embryonic and hypertrophied human ventricles but not in normal adult human ventricles. We investigated the effects of recombinant human atrial light chains (hALC-1) on the structure and enzymatic activity of synthetic filaments of ventricular myosin. The endogenous ventricular myosin light chain 1 (VLC-1) was partially replaced by recombinant hALC-1 yielding hALC-1 levels of 12%, 24% and 42%. This reconstitution of ventricular myosin with hALC-1 did not change the length of synthetic myosin filaments but led to more rounded myosin heads in comparison with those of control filaments. Actin-activated ATPase activity of myosin, a parameter of functional activity of molecular motor, amounted to 79.5 nmol P(i)/mg per min in control myosin filaments. Reconstitution with hALC-1 caused a profound increase of the actin-activated myosin ATPase activity in a dose dependent manner, for example, synthetic myosin filaments formed with 12%, 24% and 42% hALC-1 reconstituted myosin revealed the actin-activated ATPase activity increased by 18%, 26% and 36%, respectively, as compared to control. These results strongly suggest that in vivo expression of ALC-1 enhances ventricular myosin function, thereby contributing to cardiac compensation.

摘要

心房轻链1(ALC-1)在胚胎期和肥厚的人类心室中表达,但在正常成人的心室中不表达。我们研究了重组人心房轻链(hALC-1)对心室肌球蛋白合成丝的结构和酶活性的影响。用重组hALC-1部分替代内源性心室肌球蛋白轻链1(VLC-1),使hALC-1水平达到12%、24%和42%。用hALC-1对心室肌球蛋白进行这种重组并没有改变合成肌球蛋白丝的长度,但与对照丝相比,导致肌球蛋白头部更圆。肌球蛋白的肌动蛋白激活ATP酶活性是分子马达功能活性的一个参数,在对照肌球蛋白丝中为79.5 nmol P(i)/mg每分钟。用hALC-1重组导致肌动蛋白激活的肌球蛋白ATP酶活性以剂量依赖的方式显著增加,例如,与对照相比,由12%、24%和42% hALC-1重组肌球蛋白形成的合成肌球蛋白丝显示肌动蛋白激活的ATP酶活性分别增加了18%、26%和36%。这些结果强烈表明,ALC-1的体内表达增强了心室肌球蛋白的功能,从而有助于心脏代偿。

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