Requirement of Pdgfrα+ cells for calvarial bone repair

Author:

Xing Xin1ORCID,Li Zhao1,Xu Jiajia1,Chen Austin Z1,Archer Mary1,Wang Yiyun1,Xu Mingxin1,Wang Ziyi1,Zhu Manyu1,Qin Qizhi1,Thottappillil Neelima1ORCID,Zhou Myles1,James Aaron W1ORCID

Affiliation:

1. Johns Hopkins University Department of Pathology, , Baltimore, MD 21205, United States

Abstract

Abstract Platelet-derived growth factor receptor α (PDGFRα) is often considered as a general marker of mesenchymal cells and fibroblasts, but also shows expression in a portion of osteoprogenitor cells. Within the skeleton, Pdgfrα+ mesenchymal cells have been identified in bone marrow and periosteum of long bones, where they play a crucial role in participating in fracture repair. A similar examination of Pdgfrα+ cells in calvarial bone healing has not been examined. Here, we utilize Pdgfrα-CreERTM;mT/mG reporter animals to examine the contribution of Pdgfrα+ mesenchymal cells to calvarial bone repair through histology and single-cell RNA sequencing (scRNA-Seq). Results showed that Pdgfrα+ mesenchymal cells are present in several cell clusters by scRNA-Seq, and by histology a dramatic increase in Pdgfrα+ cells populated the defect site at early timepoints to give rise to healed bone tissue overtime. Notably, diphtheria toxin-mediated ablation of Pdgfrα reporter+ cells resulted in significantly impaired calvarial bone healing. Our findings suggest that Pdgfrα-expressing cells within the calvarial niche play a critical role in the process of calvarial bone repair.

Publisher

Oxford University Press (OUP)

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