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心肌细胞中的核机械感知。

Nucleus Mechanosensing in Cardiomyocytes.

机构信息

Department of Biomedical Sciences, Florida State University, Tallahassee, FL 32306, USA.

Department of Biological Science, Florida State University, Tallahassee, FL 32306, USA.

出版信息

Int J Mol Sci. 2023 Aug 28;24(17):13341. doi: 10.3390/ijms241713341.

Abstract

Cardiac muscle contraction is distinct from the contraction of other muscle types. The heart continuously undergoes contraction-relaxation cycles throughout an animal's lifespan. It must respond to constantly varying physical and energetic burdens over the short term on a beat-to-beat basis and relies on different mechanisms over the long term. Muscle contractility is based on actin and myosin interactions that are regulated by cytoplasmic calcium ions. Genetic variants of sarcomeric proteins can lead to the pathophysiological development of cardiac dysfunction. The sarcomere is physically connected to other cytoskeletal components. Actin filaments, microtubules and desmin proteins are responsible for these interactions. Therefore, mechanical as well as biochemical signals from sarcomeric contractions are transmitted to and sensed by other parts of the cardiomyocyte, particularly the nucleus which can respond to these stimuli. Proteins anchored to the nuclear envelope display a broad response which remodels the structure of the nucleus. In this review, we examine the central aspects of mechanotransduction in the cardiomyocyte where the transmission of mechanical signals to the nucleus can result in changes in gene expression and nucleus morphology. The correlation of nucleus sensing and dysfunction of sarcomeric proteins may assist the understanding of a wide range of functional responses in the progress of cardiomyopathic diseases.

摘要

心肌收缩与其他类型的肌肉收缩明显不同。在动物的整个生命周期中,心脏不断经历收缩-松弛循环。它必须在短期内在每次心跳的基础上应对不断变化的身体和能量负担,并在长期内依赖不同的机制。肌肉收缩性基于肌动蛋白和肌球蛋白的相互作用,这些作用受细胞质钙离子的调节。肌节蛋白的遗传变异可导致心脏功能障碍的病理生理发展。肌节与其他细胞骨架成分物理相连。肌动蛋白丝、微管和结蛋白负责这些相互作用。因此,来自肌节收缩的机械和生化信号被传递到心肌细胞的其他部分,并被其感知,特别是细胞核,它可以对这些刺激做出反应。锚定在核膜上的蛋白质表现出广泛的反应,重塑了细胞核的结构。在这篇综述中,我们研究了心肌细胞中机械转导的核心方面,其中机械信号向细胞核的传递可导致基因表达和细胞核形态的变化。细胞核的感知与肌节蛋白功能障碍的相关性可能有助于理解心肌病进展过程中广泛的功能反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/22e9/10487505/91593da18f6b/ijms-24-13341-g001.jpg

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