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针对软骨细胞中心代谢物对周期性压缩和剪切变形反应的分析。

Targeted analysis of chondrocyte central metabolites in response to cyclical compression and shear deformations.

作者信息

Myers Erik P, Gallagher Aurora, Welfley Avery, Battles Samuel, Gregory Aidan, Brahmachary Priyanka, Greenwood Mark, June Ronald K

机构信息

Department of Mechanical & Industrial Engineering, Montana State University, Bozeman MT.

Department of Mathematical Sciences, Montana State University, Bozeman MT.

出版信息

bioRxiv. 2025 Aug 6:2025.08.04.668582. doi: 10.1101/2025.08.04.668582.

Abstract

Osteoarthritis results in deterioration of articular cartilage, the soft tissue covering articulating surfaces of bones in joints like the knee and hip. Prior studies show that cyclical mechanical stimulation of articular cartilage results in synthesis of cartilage matrix, suggesting that therapeutic mechanical stimulation might be beneficial for cartilage repair in osteoarthritis. Several prior studies identify ion channels and cytoskeletal molecules as components of chondrocyte mechanotransduction. The pathways of central metabolism, glycolysis, the pentose phosphate pathway, and the tricarboxylic acid cycle, are necessary for producing non-essential amino acids that are needed for synthesizing matrix proteins for cartilage repair. However, it is currently unknown if and how levels of central metabolites change with applied mechanical stimulation of chondrocytes. Here, we show that applied cyclical shear and compressive deformations drive changes in multiple central metabolites. These results add to a rich picture of chondrocyte mechanotransduction including calcium signaling, ion channels, integrins, and cytoskeletal components. By finding compression- and shear-induced changes in central metabolites, these data support the potential for therapeutic mechanotransduction toward cartilage repair. Future studies may build on these results to understand the relationships between mechanical stimulation and chondrocyte central metabolism.

摘要

骨关节炎会导致关节软骨(覆盖膝关节和髋关节等关节中骨的关节面的软组织)退化。先前的研究表明,对关节软骨进行周期性机械刺激会导致软骨基质的合成,这表明治疗性机械刺激可能对骨关节炎的软骨修复有益。几项先前的研究将离子通道和细胞骨架分子确定为软骨细胞机械转导的组成部分。中央代谢途径、糖酵解、磷酸戊糖途径和三羧酸循环对于产生合成软骨修复所需基质蛋白所需的非必需氨基酸是必要的。然而,目前尚不清楚中央代谢物的水平是否以及如何随着对软骨细胞施加机械刺激而发生变化。在这里,我们表明施加的周期性剪切和压缩变形会驱动多种中央代谢物的变化。这些结果丰富了软骨细胞机械转导的图景,包括钙信号传导、离子通道、整合素和细胞骨架成分。通过发现中央代谢物中由压缩和剪切引起的变化,这些数据支持了治疗性机械转导促进软骨修复的潜力。未来的研究可能会基于这些结果来理解机械刺激与软骨细胞中央代谢之间的关系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4d24/12340845/9639d002c228/nihpp-2025.08.04.668582v1-f0001.jpg

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