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通过分析加载诱导的细胞死亡来量化软骨的多孔弹性材料特性。

Quantification of Cartilage Poroelastic Material Properties Via Analysis of Loading-Induced Cell Death.

机构信息

Department of Biomedical Engineering, University of Rochester, Rochester, NY 14627.

University of Rochester.

出版信息

J Biomech Eng. 2024 Aug 1;146(8). doi: 10.1115/1.4065194.

Abstract

Articular cartilage (AC) is a load-bearing tissue that covers long bones in synovial joints. The biphasic/poroelastic mechanical properties of AC help it to protect joints by distributing loads, absorbing impact forces, and reducing friction. Unfortunately, alterations in these mechanical properties adversely impact cartilage function and precede joint degeneration in the form of osteoarthritis (OA). Thus, understanding what factors regulate the poroelastic mechanical properties of cartilage is of great scientific and clinical interest. Transgenic mouse models provide a valuable platform to delineate how specific genes contribute to cartilage mechanical properties. However, the poroelastic mechanical properties of murine articular cartilage are challenging to measure due to its small size (thickness ∼ 50 microns). In the current study, our objective was to test whether the poroelastic mechanical properties of murine articular cartilage can be determined based solely on time-dependent cell death measurements under constant loading conditions. We hypothesized that in murine articular cartilage subjected to constant, sub-impact loading from an incongruent surface, cell death area and tissue strain are closely correlated. We further hypothesized that the relationship between cell death area and tissue strain can be used-in combination with inverse finite element modeling-to compute poroelastic mechanical properties. To test these hypotheses, murine cartilage-on-bone explants from different anatomical locations were subjected to constant loading conditions by an incongruent surface in a custom device. Cell death area increased over time and scaled linearly with strain, which rose in magnitude over time due to poroelastic creep. Thus, we were able to infer tissue strain from cell death area measurements. Moreover, using tissue strain values inferred from cell death area measurements, we applied an inverse finite element modeling procedure to compute poroelastic material properties and acquired data consistent with previous studies. Collectively, our findings demonstrate in the key role poroelastic creep plays in mediating cell survival in mechanically loaded cartilage and verify that cell death area can be used as a surrogate measure of tissue strain that enables determination of murine cartilage mechanical properties.

摘要

关节软骨(AC)是一种覆盖滑膜关节长骨的承重组织。AC 的双相/多孔弹性力学特性有助于通过分布载荷、吸收冲击力和减少摩擦来保护关节。不幸的是,这些力学特性的改变会对软骨功能产生不利影响,并以前骨关节炎(OA)的形式导致关节退化。因此,了解哪些因素调节软骨的多孔弹性力学特性具有重要的科学和临床意义。转基因小鼠模型为阐明特定基因如何影响软骨力学特性提供了有价值的平台。然而,由于其体积小(厚度约为 50 微米),测量鼠关节软骨的多孔弹性力学特性具有挑战性。在本研究中,我们的目的是测试在恒定载荷条件下仅基于时变细胞死亡测量是否可以确定鼠关节软骨的多孔弹性力学特性。我们假设,在受到来自不匹配表面的恒定亚冲击载荷的鼠关节软骨中,细胞死亡面积和组织应变密切相关。我们进一步假设,细胞死亡面积与组织应变之间的关系可以与逆有限元建模结合使用,以计算多孔弹性力学特性。为了验证这些假设,我们使用定制设备,通过不匹配表面对来自不同解剖位置的鼠软骨-骨标本施加恒定载荷条件。细胞死亡面积随时间增加并与应变呈线性关系,由于多孔弹性蠕变,应变随时间增大。因此,我们能够从细胞死亡面积测量中推断出组织应变。此外,我们使用从细胞死亡面积测量中推断出的组织应变值,应用逆有限元建模程序计算多孔弹性材料特性,并获得与先前研究一致的数据。总的来说,我们的研究结果表明,多孔弹性蠕变在介导机械加载软骨中的细胞存活中起着关键作用,并验证了细胞死亡面积可以作为组织应变的替代测量值,从而确定鼠软骨的力学特性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/59a3/11080949/131ed61a877e/BIO-23-1178_graphical-image.jpg

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