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利用双折射评估平滑肌中的细丝晶格变化。

Filament lattice changes in smooth muscle assessed using birefringence.

作者信息

Smolensky A V, Ford L E

机构信息

Kranner Institute of Cardiology, Indiana University School of Medicine, Indianapolis, IN 46202, USA.

出版信息

Can J Physiol Pharmacol. 2005 Oct;83(10):933-40. doi: 10.1139/y05-095.

Abstract

The long functional range of some types of smooth muscle has been the subject of recent study. It has been proposed that the muscle filament lattice adapts to longer lengths by placing more filaments in series and that lattice plasticity is facilitated by myosin filament evanescence, with filaments dissociating during relaxation and reforming upon activation. Support for these dynamic changes in the filament lattice has been provided partly by changes in contractile parameters at different times in the contraction-relaxation cycle at different lengths. If the changes in contractile parameters result from filament formation and dissociation, these structural changes must occur on the time scale of tension development and relaxation. To assess whether thick-filament formation could account for the contractile changes, we measured birefringence continuously during activation and relaxation and compared these optical changes with the time course of force development and relaxation. Birefringence is a well-known property of muscle; striations in skeletal and cardiac muscle result from the A-bands being anisotropic, i.e., birefringent, and it is now known that this optical property is due to the presence of myosin thick filaments in the A-bands. Thus, the strength of birefringence is expected to represent the density of thick filaments. Here, we describe the principle of the method, the techniques for recording the optical signals, some initial results, and discuss the interpretation of results and some limitations of the method.

摘要

某些类型平滑肌的长功能范围一直是近期研究的主题。有人提出,肌丝晶格通过串联更多的肌丝来适应更长的长度,并且肌球蛋白丝的消失促进了晶格可塑性,即丝在松弛过程中解离,在激活时重新形成。在不同长度的收缩 - 舒张周期的不同时间点,收缩参数的变化为肌丝晶格的这些动态变化提供了部分支持。如果收缩参数的变化是由丝的形成和解离引起的,那么这些结构变化必定发生在张力发展和松弛的时间尺度上。为了评估粗肌丝的形成是否可以解释收缩变化,我们在激活和松弛过程中连续测量双折射,并将这些光学变化与力发展和松弛的时间过程进行比较。双折射是肌肉的一个众所周知的特性;骨骼肌和心肌中的条纹是由于A带具有各向异性,即双折射,现在已知这种光学特性是由于A带中存在肌球蛋白粗肌丝。因此,双折射的强度有望代表粗肌丝的密度。在此,我们描述该方法的原理、记录光学信号的技术、一些初步结果,并讨论结果的解释以及该方法的一些局限性。

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