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The biological basis of degenerative disc disease: proteomic and biomechanical analysis of the canine intervertebral disc

机译:退行性椎间盘疾病的生物学基础:犬椎间盘的蛋白质组学和生物力学分析

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Introduction: In the present study, we sought to quantify and contrast the secretome and biomechanical properties of the non-chondrodystrophic (NCD) and chondrodystrophic (CD) canine intervertebral disc (IVD) nucleus pulposus (NP). Methods: We used iTRAQ proteomic methods to quantify the secretome of both CD and NCD NP. Differential levels of proteins detected were further verified using immunohistochemistry, Western blotting, and proteoglycan extraction in order to evaluate the integrity of the small leucine-rich proteoglycans (SLRPs) decorin and biglycan. Additionally, we used robotic biomechanical testing to evaluate the biomechanical properties of spinal motion segments from both CD and NCD canines. Results: We detected differential levels of decorin, biglycan, and fibronectin, as well as of other important extracellular matrix (ECM)-related proteins, such as fibromodulin and HAPLN1 in the IVD NP obtained from CD canines compared with NCD canines. The core proteins of the vital SLRPs decorin and biglycan were fragmented in CD NP but were intact in the NP of the NCD animals. CD and NCD vertebral motion segments demonstrated significant differences, with the CD segments having less stiffness and a more varied range of motion. Conclusions: The CD NP recapitulates key elements of human degenerative disc disease. Our data suggest that at least some of the compromised biomechanical properties of the degenerative disc arise from fibrocartilaginous metaplasia of the NP secondary to fragmentation of SLRP core proteins and associated degenerative changes affecting the ECM. This study demonstrates that the degenerative changes that naturally occur within the CD NP make this animal a valuable animal model with which to study IVD degeneration and potential biological therapeutics.
机译:介绍:在本研究中,我们寻求量化和对比非脑脊育(NCD)和软骨育(CD)犬椎间盘(IVD)髓核(NP)的秘密和生物力学特性。方法:我们使用ITRAQ蛋白质组学方法来量化CD和NCD NP的秘密。使用免疫组织化学,蛋白质印迹和蛋白多糖提取进一步验证检测到检测到的差异水平,以评估小亮氨酸富含蛋白质糖化合物(SLRPS)装饰蛋白和Biglycan的完整性。此外,我们使用机器人生物力学测试来评估来自CD和NCD犬的脊柱运动段的生物力学特性。结果:我们检测到差异水平的装饰素,大碳和纤连蛋白,以及其他重要的细胞外基质(ECM)相关蛋白,如纤维蛋白和HAPLN1,与NCD犬的IVD NP中获得的IVD NP中。重要的SLRPS DECORIN和BIGLYCAN的核心蛋白在CD NP中裂片,但在NCD动物的NP中完整。 CD和NCD椎体运动段呈现显着差异,CD段具有较小的刚度和更多样化的运动。结论:CD NP概括了人退行性椎间盘疾病的关键要素。我们的数据表明,退行性椎间盘的至少一些受损的生物力学性质来自二次NP的纤维纤维状的细胞,与SLRP核心蛋白的破碎和影响ECM的相关退行性变化。本研究表明,在CD NP内天然发生的退行性变化使得这种动物成为有价值的动物模型,用于研究IVD退化和潜在的生物治疗。

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