Distinct fibroblast progenitor subpopulation expedites regenerative mucosal healing by immunomodulation

Author:

Ko Kang I.12ORCID,DerGarabedian Brett P.1ORCID,Chen Zhaoxu1ORCID,Debnath Rahul1ORCID,Ko Annette1ORCID,Link Brittany N.1ORCID,Korostoff Jonathan M.1ORCID,Graves Dana T.1ORCID

Affiliation:

1. Department of Periodontics, School of Dental Medicine, University of Pennsylvania 1 , Philadelphia, PA, USA

2. Center for Innovation and Precision Dentistry, School of Dental Medicine, University of Pennsylvania 2 , Philadelphia, PA, USA

Abstract

Injuries that heal by fibrosis can compromise organ function and increase patient morbidity. The oral mucosal barrier has a high regenerative capacity with minimal scarring, but the cellular mechanisms remain elusive. Here, we identify distinct postnatal paired-related homeobox-1+ (Prx1+) cells as a critical fibroblast subpopulation that expedites mucosal healing by facilitating early immune response. Using transplantation and genetic ablation model in mice, we show that oral mucosa enriched with Prx1+ cells heals faster than those that lack Prx1+ cells. Lineage tracing and scRNA-seq reveal that Prx1+ fibroblasts exhibit progenitor signatures in physiologic and injured conditions. Mechanistically, Prx1+ progenitors accelerate wound healing by differentiating into immunomodulatory SCA1+ fibroblasts, which prime macrophage recruitment through CCL2 as a key part of pro-wound healing response. Furthermore, human Prx1+ fibroblasts share similar gene and spatial profiles compared to their murine counterpart. Thus, our data suggest that Prx1+ fibroblasts may provide a valuable source in regenerative procedures for the treatment of corneal wounds and enteropathic fibrosis.

Funder

National Institute of Dental and Craniofacial Research

Publisher

Rockefeller University Press

Subject

Immunology,Immunology and Allergy

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