Spatially defined single-cell transcriptional profiling characterizes diverse chondrocyte subtypes and nucleus pulposus progenitors in human intervertebral discs

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摘要A comprehensive understanding of the cellular heterogeneity and molecular mechanisms underlying the development,homeostasis, and disease of human intervertebral disks (IVDs) remains challenging. Here, the transcriptomic landscape of 108108 IVD cells was mapped using single-cell RNA sequencing of three main compartments from young and adult healthy IVDs, including the nucleus pulposus (NP), annulus fibrosus, and cartilage endplate (CEP). The chondrocyte subclusters were classified based on their potential regulatory, homeostatic, and effector functions in extracellular matrix (ECM) homeostasis. Notably, in the NP, a PROCR+ resident progenitor population showed enriched colony-forming unit-fibroblast (CFU-F) activity and trilineage differentiation capacity. Finally, intercellular crosstalk based on signaling network analysis uncovered that the PDGF and TGF-β cascades are important cues in the NP microenvironment. In conclusion, a single-cell transcriptomic atlas that resolves spatially regulated cellular heterogeneity together with the critical signaling that underlies homeostasis will help to establish new therapeutic strategies for IVD degeneration in the clinic.

作者 Yibo Gan ^[1] Jian He ^[2] Jun Zhu ^[3] Zhengyang Xu ^[2] Zhong Wang ^[3] Jing Yan ^[2] Ou Hu ^[3] Zhijie Bai ^[2] Lin Chen ^[4] Yangli Xie ^[4] Min Jin ^[4] Shuo Huang ^[4] Bing Liu ^[5] Peng Liu ^[1] 学术成果认领

作者单位 Department of Spine Surgery,Center of Orthopedics,Daping Hospital,Army Medical University(Third Military Medical University),Chongqing,China;State Key Laboratory of Trauma,Burns and Combined Injury,Army Medical University(Third Military Medical University),Chongqing,China ^[1] State Key Laboratory of Proteomics,Academy of Military Medical Sciences,Academy of Military Sciences,Beijing,China ^[2] Department of Spine Surgery,Center of Orthopedics,Daping Hospital,Army Medical University(Third Military Medical University),Chongqing,China ^[3] Center of Bone Metabolism and Repair,State Key Laboratory of Trauma,Burns and Combined Injury,Trauma Center,Research Institute of Surgery,Laboratory for the Prevention and Rehabilitation of Military Training Related Injuries,Daping Hospital,Army Medical University(Third Military Medical University),Chongqing,China ^[4] State Key Laboratory of Proteomics,Academy of Military Medical Sciences,Academy of Military Sciences,Beijing,China;State Key Laboratory of Experimental Hematology,Institute of Hematology,Fifth Medical Center of Chinese PLA General Hospital,Beijing,China;Key Laboratory for Regenerative Medicine of Ministry of Education,Institute of Hematology,School of Medicine,Jinan University,Guangzhou,China ^[5]

栏目名称 ORIGINAL ARTICLES

发布时间 2021-11-01

基金项目

The authors thank Hongxia Hu and Haitao Hu from Berry Genomics for technical support with scRNA-seq The authors acknowledge Zhigang Zhou and Feng Wei from Peking University Third Hospital and Fei Luo,Bo Yu,Bo Huang,Qizhao Huang,Qinghua Ma,and Ruili Cai from Army Medical University for their excellent technical support with sample collection and single-cell preparation The authors are grateful to Wenxia Zheng and Hengsheng Tao from Olympus and Xue Yang and Qing Zhou from Army Medical University for help with section staining and imaging This study was supported by grants from the National Natural Science Foundation of China National Key Research and Development Program of China Training Plan of Talents'Innovation of Army Medical Center of PLA Postdoctoral Innovative Talent Support Program in Chongqing and Fund for Excellent Young Scholars of the State Key Laboratory of Trauma,Burns and Combined Injury

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