CD51 labels periosteal injury-responsive osteoprogenitors

Ye Cao; Ivo Kalajzic; Brya G Matthews

doi:10.3389/fphys.2023.1231352

CD51 labels periosteal injury-responsive osteoprogenitors

Front Physiol. 2023 Sep 4:14:1231352. doi: 10.3389/fphys.2023.1231352. eCollection 2023.

Authors

Ye Cao¹, Ivo Kalajzic², Brya G Matthews^{1

2}

Affiliations

¹ Department of Molecular Medicine and Pathology, University of Auckland, Auckland, New Zealand.
² Center for Regenerative Medicine and Skeletal Development, School of Dental Medicine, UConn Health, Farmington, CT, United States.

Abstract

The periosteum is a critical source of skeletal stem and progenitor cells (SSPCs) that form callus tissue in response to injury. There is yet to be a consensus on how to identify SSPCs in the adult periosteum. The aim of this study was to understand how potential murine periosteal SSPC populations behave in vivo and in response to injury. We evaluated the in vivo differentiation potential of Sca1^-CD51⁺ and Sca1⁺CD51⁺ cells following transplantation. In vitro, the Sca1⁺CD51⁺ population appears to be more primitive multipotent cells, but after transplantation, Sca1^-CD51⁺ cells showed superior engraftment, expansion, and differentiation into chondrocytes and osteoblasts. Despite representing a clear population with flow cytometry, we identified very few Sca1⁺CD51⁺ cells histologically. Using a periosteal scratch injury model, we successfully mimicked the endochondral-like healing process seen in unstable fractures, including the expansion and osteochondral differentiation of αSMA⁺ cells following injury. CD51⁺ cells were present in the cambium layer of resting periosteum and expanded following injury. Sca1⁺CD51^- cells were mainly localized in the outer periosteal layer. We found that injury increased colony-forming unit fibroblast (CFU-F) formation in the periosteum and led to rapid expansion of CD90⁺ cells. Several other populations, including Sca1^-CD51⁺ and CD34⁺ cells, were expanded by day 7. Mice with enhanced fracture healing due to elevated Notch signaling mediated by NICD1 overexpression showed significant expansion of CD51⁺ and CD34^hi cells in the early stages of healing, suggesting these populations contribute to more rapid healing. In conclusion, we demonstrate that periosteal injury leads to the expansion of various SSPC populations, but further studies are required to confirm their lineage hierarchy in the adult skeletal system. Our data indicate that CD51⁺ skeletal progenitor cells are injury-responsive and show good engraftment and differentiation potential upon transplantation.

Keywords: CD34; CD51; Notch; SCA1; fracture; periosteum.

Grants and funding

R01 AR055607/AR/NIAMS NIH HHS/United States