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横纹肌肌节结构完整性:肌节 Z 盘的自动化分析。

Striated myocyte structural integrity: Automated analysis of sarcomeric z-discs.

机构信息

Center for Complex Biological Systems, University of California, Irvine, Irvine, California, United States of America.

Edwards Lifesciences Center for Advanced Cardiovascular Technology, University of California, Irvine, Irvine, California, United States of America.

出版信息

PLoS Comput Biol. 2020 Mar 4;16(3):e1007676. doi: 10.1371/journal.pcbi.1007676. eCollection 2020 Mar.

Abstract

As sarcomeres produce the force necessary for contraction, assessment of sarcomere order is paramount in evaluation of cardiac and skeletal myocytes. The uniaxial force produced by sarcomeres is ideally perpendicular to their z-lines, which couple parallel myofibrils and give cardiac and skeletal myocytes their distinct striated appearance. Accordingly, sarcomere structure is often evaluated by staining for z-line proteins such as α-actinin. However, due to limitations of current analysis methods, which require manual or semi-manual handling of images, the mechanism by which sarcomere and by extension z-line architecture can impact contraction and which characteristics of z-line architecture should be used to assess striated myocytes has not been fully explored. Challenges such as isolating z-lines from regions of off-target staining that occur along immature stress fibers and cell boundaries and choosing metrics to summarize overall z-line architecture have gone largely unaddressed in previous work. While an expert can qualitatively appraise tissues, these challenges leave researchers without robust, repeatable tools to assess z-line architecture across different labs and experiments. Additionally, the criteria used by experts to evaluate sarcomeric architecture have not been well-defined. We address these challenges by providing metrics that summarize different aspects of z-line architecture that correspond to expert tissue quality assessment and demonstrate their efficacy through an examination of engineered tissues and single cells. In doing so, we have elucidated a mechanism by which highly elongated cardiomyocytes become inefficient at producing force. Unlike previous manual or semi-manual methods, characterization of z-line architecture using the metrics discussed and implemented in this work can quantitatively evaluate engineered tissues and contribute to a robust understanding of the development and mechanics of striated muscles.

摘要

由于肌节产生收缩所需的力,评估肌节的有序性对于评估心肌和骨骼肌细胞至关重要。肌节产生的单轴力理想上垂直于它们的 Z 线,Z 线将平行的肌原纤维连接起来,使心肌和骨骼肌呈现出独特的条纹外观。因此,肌节结构通常通过染色 Z 线蛋白(如α-辅肌动蛋白)来评估。然而,由于当前分析方法的局限性,这些方法需要手动或半自动处理图像,因此肌节和 Z 线结构如何影响收缩以及应该使用 Z 线结构的哪些特征来评估条纹状肌细胞的机制尚未得到充分探索。以前的工作中,尚未解决诸如从沿未成熟的应激纤维和细胞边界的非目标染色区域分离 Z 线以及选择用于总结整体 Z 线结构的指标等挑战。虽然专家可以定性评估组织,但这些挑战使研究人员缺乏在不同实验室和实验中评估 Z 线结构的稳健、可重复的工具。此外,专家用于评估肌节结构的标准尚未得到很好的定义。我们通过提供可总结 Z 线结构不同方面的指标来解决这些挑战,这些指标与专家对组织质量的评估相对应,并通过对工程组织和单细胞的检查来证明其有效性。通过这样做,我们阐明了一个机制,即高度拉长的心肌细胞在产生力方面变得效率低下。与以前的手动或半自动方法不同,使用本文讨论和实施的指标对 Z 线结构进行特征描述可以定量评估工程组织,并有助于深入了解条纹肌肉的发育和力学特性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bb1c/7075639/c9965c581d27/pcbi.1007676.g001.jpg

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