Age-dependent changes in intervertebral disc cell mitochondria and bioenergetics.

IF 3.2 3区 医学 Q3 CELL & TISSUE ENGINEERING European cells & materials Pub Date : 2018-10-18 DOI:10.22203/eCM.v036a13
R Hartman, P Patil, R Tisherman, C St Croix, L J Niedernhofer, P D Robbins, F Ambrosio, B Van Houten, G Sowa, N Vo
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Abstract

Robust cellular bioenergetics is vital in the energy-demanding process of maintaining matrix homeostasis in the intervertebral disc. Age-related decline in disc cellular bioenergetics is hypothesised to contribute to the matrix homeostatic perturbation observed in intervertebral disc degeneration. The present study aimed to measure how ageing impacted disc cell mitochondria and bioenergetics. Age-related changes measured included matrix content and cellularity in disc tissue, as well as matrix synthesis, cell proliferation and senescence markers in cell cultures derived from annulus fibrosus (AF) and nucleus pulposus (NP) isolated from the discs of young (6-9 months) and older (36-50 months) New Zealand White rabbits. Cellular bioenergetic parameters were measured using a Seahorse XFe96 Analyzer, in addition to quantitating mitochondrial morphological changes and membrane potential. Ageing reduced mitochondrial number and membrane potential in both cell types. Also, it significantly reduced glycolytic capacity, mitochondrial reserve capacity, maximum aerobic capacity and non-glucose-dependent respiration in NP. Moreover, NP cells exhibited age-related decline in matrix synthesis and reduced cellularity in older tissues. Despite a lack of changes in mitochondrial respiration with age, AF cells showed an increase in glycolysis and altered matrix production. While previous studies report age-related matrix degenerative changes in disc cells, the present study revealed, for the first time, that ageing affected mitochondrial number and function, particularly in NP cells. Consequently, age-related bioenergetic changes may contribute to the functional alterations in aged NP cells that underlie disc degeneration.

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椎间盘细胞线粒体和生物能随年龄的变化而变化。
在维持椎间盘基质平衡的能量需求过程中,强大的细胞生物能至关重要。与年龄相关的椎间盘细胞生物能下降被认为是导致椎间盘退变的基质平衡紊乱的原因之一。本研究旨在测量衰老如何影响椎间盘细胞线粒体和生物能。所测量的与年龄相关的变化包括椎间盘组织中的基质含量和细胞度,以及从年轻(6-9 个月)和年长(36-50 个月)新西兰白兔椎间盘中分离出来的纤维环(AF)和髓核(NP)细胞培养物中的基质合成、细胞增殖和衰老标记物。除了量化线粒体形态变化和膜电位外,还使用海马 XFe96 分析仪测量了细胞生物能参数。老化降低了两种细胞的线粒体数量和膜电位。此外,老化还明显降低了 NP 细胞的糖酵解能力、线粒体储备能力、最大有氧能力和非葡萄糖依赖性呼吸。此外,NP 细胞表现出与年龄相关的基质合成能力下降,并降低了老组织的细胞性。尽管线粒体呼吸没有随着年龄的增长而发生变化,但 AF 细胞却显示出糖酵解的增加和基质生成的改变。虽然之前的研究报告了椎间盘细胞中与年龄相关的基质退行性变化,但本研究首次揭示了衰老会影响线粒体的数量和功能,尤其是在 NP 细胞中。因此,与年龄相关的生物能变化可能是导致椎间盘退化的老化 NP 细胞功能改变的原因。
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来源期刊
European cells & materials
European cells & materials 生物-材料科学:生物材料
CiteScore
6.00
自引率
6.50%
发文量
55
审稿时长
1.5 months
期刊介绍: eCM provides an interdisciplinary forum for publication of preclinical research in the musculoskeletal field (Trauma, Maxillofacial (including dental), Spine and Orthopaedics). The clinical relevance of the work must be briefly mentioned within the abstract, and in more detail in the paper. Poor abstracts which do not concisely cover the paper contents will not be sent for review. Incremental steps in research will not be entertained by eCM journal.Cross-disciplinary papers that go across our scope areas are welcomed.
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