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Serglycin secreted by late-stage nucleus pulposus cells is a biomarker of intervertebral disc degeneration

Fan Chen, Linchuan Lei, Shunlun Chen, Zhuoyang Zhao, Yuming Huang, Guowei Jiang, Xingyu Guo, Zemin Li, Zhaomin Zheng, Jianru Wang

2024Nature Communications73 citationsDOIOpen Access PDF

Abstract

Intervertebral disc degeneration is a natural process during aging and a leading cause of lower back pain. Here, we generate a comprehensive atlas of nucleus pulposus cells using single-cell RNA-seq analysis of human nucleus pulposus tissues (three males and four females, age 41.14 ± 18.01 years). We identify fibrotic late-stage nucleus pulposus cells characterized by upregulation of serglycin expression which facilitate the local inflammatory response by promoting the infiltration of inflammatory cytokines and macrophages. Finally, we discover that daphnetin, a potential serglycin ligand, substantially mitigates the local inflammatory response by downregulating serglycin expression in an in vivo mouse model, thus alleviating intervertebral disc degeneration. Taken together, we identify late-stage nucleus pulposus cells and confirm the potential mechanism by which serglycin regulates intervertebral disc degeneration. Our findings indicate that serglycin is a latent biomarker of intervertebral disc degeneration and may contribute to development of diagnostic and therapeutic strategies.

Topics & Concepts

Intervertebral discNucleusDegeneration (medical)Downregulation and upregulationPathologyBiomarkerCell biologyInflammationMedicineIn vivoBiologyAnatomyImmunologyGeneBiochemistryBiotechnologySpine and Intervertebral Disc PathologyMusculoskeletal pain and rehabilitationOsteoarthritis Treatment and Mechanisms