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一项体外研究,旨在深入了解 MMPs-1 和 MMPs-9 对关节软骨生物力学性能的协同作用。

An in vitro investigation to understand the synergistic role of MMPs-1 and 9 on articular cartilage biomechanical properties.

机构信息

Department of Mechanical Engineering, University of Louisiana at Lafayette, Lafayette, LA, 70503, USA.

Department of Biology, University of Louisiana at Lafayette, Lafayette, LA, 70503, USA.

出版信息

Sci Rep. 2021 Jul 13;11(1):14409. doi: 10.1038/s41598-021-93744-1.

Abstract

Matrix metalloproteinases (MMPs) play a crucial role in enzymatically digesting cartilage extracellular matrix (ECM) components, resulting in degraded cartilage with altered mechanical loading capacity. Overexpression of MMPs is often caused by trauma, physiologic conditions and by disease. To understand the synergistic impact MMPs have on cartilage biomechanical properties, MMPs from two subfamilies: collagenase (MMP-1) and gelatinase (MMP-9) were investigated in this study. Three different ratios of MMP-1 (c) and MMP-9 (g), c1:g1, c3:g1 and c1:g3 were considered to develop a degradation model. Thirty samples, harvested from bovine femoral condyles, were treated in groups of 10 with one concentration of enzyme mixture. Each sample was tested in a healthy state prior to introducing degradative enzymes to establish a baseline. Samples were subjected to indentation loading up to 20% bulk strain. Both control and treated samples were mechanically and histologically assessed to determine the impact of degradation. Young's modulus and peak load of the tissue under indentation were compared between the control and degraded cartilage explants. Cartilage degraded with the c3:g1 enzyme concentration resulted in maximum 33% reduction in stiffness and peak load compared to the other two concentrations. The abundance of collagenase is more responsible for cartilage degradation and reduced mechanical integrity.

摘要

基质金属蛋白酶(MMPs)在酶解软骨细胞外基质(ECM)成分方面发挥着关键作用,导致软骨降解并改变机械承载能力。MMPs 的过度表达通常由创伤、生理状况和疾病引起。为了了解 MMPs 对软骨生物力学特性的协同影响,本研究中研究了两个亚家族的 MMPs:胶原酶(MMP-1)和明胶酶(MMP-9)。研究了三种不同比例的 MMP-1(c)和 MMP-9(g),即 c1:g1、c3:g1 和 c1:g3,以建立降解模型。从牛股骨髁中收获了 30 个样本,分为 10 组,用一种酶混合物浓度进行处理。每个样本在引入降解酶之前都在健康状态下进行测试,以建立基线。样本在达到 20%整体应变的情况下进行压痕加载。对对照和处理样本进行机械和组织学评估,以确定降解的影响。比较了压痕下组织的杨氏模量和峰值载荷,以评估对照和降解软骨样本之间的差异。与其他两种浓度相比,c3:g1 酶浓度下降解的软骨导致刚度和峰值载荷最大降低 33%。胶原酶的丰度更负责软骨降解和机械完整性的降低。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0e1d/8277889/e75ff1d1dc39/41598_2021_93744_Fig1_HTML.jpg

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