Macrophage Changes and High‐Throughput Sequencing in Aging Mouse Intervertebral Disks

Macrophage Changes and High‐Throughput Sequencing in Aging Mouse Intervertebral Disks

ABSTRACT Background Intervertebral disk (IVD) degeneration is associated with lower back pain and aging; however, the mechanisms underlying age‐related changes and the changes in macrophage polarization in aging intervertebral disks require further elucidation. The aim of this study was to evaluate...

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Main Authors: Wei Wang, Cheng Jiang, Jiong‐Hui Chen, Yong‐Long Chen, Zhen‐Wu Zhang, Zhi‐Chao Yang, Jun Li, Xiao‐Chuan Li
Format: Article
Language:English
Published: Wiley 2025-06-01
Series:JOR Spine
Subjects:
high‐throughput sequencing
intervertebral disk
macrophages
senescence
Online Access:https://doi.org/10.1002/jsp2.70061
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Summary:ABSTRACT Background Intervertebral disk (IVD) degeneration is associated with lower back pain and aging; however, the mechanisms underlying age‐related changes and the changes in macrophage polarization in aging intervertebral disks require further elucidation. The aim of this study was to evaluate changes in macrophages, the differential expression of senescence genes, and their relationship with hub genes in IVDs during aging in mice. Methods Twenty‐eight male wild C57 mice aged 4 weeks were divided into two groups. Four mice per group were selected for high‐throughput sequencing and 10 for tail IVD immunohistochemical analysis. Adult and aged mouse IVD specimens were stained with hematoxylin–eosin, Fast Green, and Alcian Blue to determine collagen (Col) 1, Col2, proteoglycan, P16, P21, P53, CD11b, CD86, CD206, IL‐1, TGF‐β, and IL‐4 expression. High‐throughput sequencing was performed on adult and aged mouse IVD tissues. Results Aged mouse IVDs showed reduced height and marked degeneration, with decreased Col2 and proteoglycan expression and increased Col1 expression. The expression of senescence markers, senescence‐associated IL‐1, TGF‐β, and IL‐4, and macrophage‐related markers, CD11b, CD86, and CD206, increased markedly with age. High‐throughput sequencing revealed 1975 differentially expressed genes in adult and aged mice, with 797 genes showing upregulated expression (top five: Kcna7, Mmp9, Panx3, Myl10, and Bglap) and 1178 showing downregulated expression (top five: Srd5a2, Slc38a5, Gm47283, Npy, and Pcdh8). Gene Ontology and pathway enrichment analyses highlighted aging‐related cellular components, biological processes, and metabolic pathways. The identified hub genes included Cox5a, Ndufs6, and Ndufb9. Conclusions Disk senescence and reduced height in aged mice are linked to upregulated expression of senescence‐associated phenotypes and macrophage polarization markers. These findings suggest that macrophages and differential gene expression play key roles in age‐related IVD degeneration, indicating that they can be used as potential targets for therapeutic intervention.
ISSN:2572-1143

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