Characterization of the Nucleus Pulposus Progenitor Cells via Spatial Transcriptomics

Author:

Chen Yu12,Zhang Long12,Shi Xueqing12,Han Jie12,Chen Jingyu3,Zhang Xinya4,Xie Danlin45,Li Zan12,Niu Xing6,Chen Lijie6,Yang Chaoyong7,Sun Xiujie8,Zhou Taifeng9,Su Peiqiang9,Li Na12,Greenblatt Matthew B.1011,Ke Rongqin4,Huang Jianming12,Chen Zhe‐Sheng13,Xu Ren12ORCID

Affiliation:

1. The First Affiliated Hospital of Xiamen University‐ICMRS Collaborating Center for Skeletal Stem Cells State Key Laboratory of Cellular Stress Biology Faculty of Medicine and Life Sciences School of Medicine Xiamen University Xiamen 361102 China

2. Xiamen Key Laboratory of Regeneration Medicine Fujian Provincial Key Laboratory of Organ and Tissue Regeneration School of Medicine Xiamen University Xiamen 361102 China

3. Gene Denovo Biotechnology Co Guangzhou 510006 China

4. School of Medicine and School of Biomedical Sciences Huaqiao University Quanzhou 362000 China

5. School of Life Sciences Westlake University Hangzhou 310030 China

6. China Medical University Shenyang Liaoning 110122 China

7. Department of Chemical Biology College of Chemistry and Chemical Engineering Xiamen University Xiamen 361005 China

8. Department of Obstetrics and Gynecology School of Medicine Xiang'an Hospital of Xiamen University Xiamen University Xiamen 361102 China

9. Department of Spine Surgery Guangdong Provincial Key Laboratory of Orthopedics and Traumatology The First Affiliated Hospital of Sun Yat‐sen University Guangzhou 510080 China

10. Department of Pathology and Laboratory Medicine Weill Cornell Medical College New York NY 10065 USA

11. Research Division Hospital for Special Surgery New York NY 10065 USA

12. Department of Orthopedics Chengong Hospital (the 73th Group Military Hospital of People's Liberation Army) affiliated to Xiamen University Xiamen 361000 China

13. College of Pharmacy and Health Sciences St. John's University New York NY 11439 USA

Abstract

AbstractLoss of refreshment in nucleus pulposus (NP) cellularity leads to intervertebral disc (IVD) degeneration. Nevertheless, the cellular sequence of NP cell differentiation remains unclear, although an increasing body of literature has identified markers of NP progenitor cells (NPPCs). Notably, due to their fragility, the physical enrichment of NP‐derived cells has limited conventional transcriptomic approaches in multiple studies. To overcome this limitation, a spatially resolved transcriptional atlas of the mouse IVD is generated via the 10x Genomics Visium platform dividing NP spots into two clusters. Based on this, most reported NPPC‐markers, including Cathepsin K (Ctsk), are rare and predominantly located within the NP‐outer subset. Cell lineage tracing further evidence that a small number of Ctsk‐expressing cells generate the entire adult NP tissue. In contrast, Tie2, which has long suggested labeling NPPCs, is actually neither expressed in NP subsets nor labels NPPCs and their descendants in mouse models; consistent with this, an in situ sequencing (ISS) analysis validated the absence of Tie2 in NP tissue. Similarly, no Tie2‐cre‐mediated labeling of NPPCs is observed in an IVD degenerative mouse model. Altogether, in this study, the first spatial transcriptomic map of the IVD is established, thereby providing a public resource for bone biology.

Funder

National Natural Science Foundation of China

National Key Research and Development Program of China

Natural Science Foundation of Fujian Province

Publisher

Wiley

Subject

General Physics and Astronomy,General Engineering,Biochemistry, Genetics and Molecular Biology (miscellaneous),General Materials Science,General Chemical Engineering,Medicine (miscellaneous)

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