Identification of LRP1+CD13+ human periosteal stem cells that require LRP1 for bone repair
Youngjae Jeong, Lorenzo Deveza, Laura Ortinau, Kevin Lei, John R. Dawson, Dongsu Park
Youngjae Jeong, Lorenzo Deveza, Laura Ortinau, Kevin Lei, John R. Dawson, Dongsu Park
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Research Article Bone biology Stem cells

Identification of LRP1+CD13+ human periosteal stem cells that require LRP1 for bone repair

Abstract

Human periosteal skeletal stem cells (P-SSCs) are critical for cortical bone maintenance and repair. However, their in vivo identity, molecular characteristics, and specific markers remain unknown. Here, single-cell sequencing revealed human periosteum contains SSC clusters expressing known SSC markers, podoplanin (PDPN) and PDGFRA. Notably, human P-SSCs, but not bone marrow SSCs, selectively expressed identified markers low density lipoprotein receptor-related protein 1 (LRP1) and CD13. These LRP1+CD13+ human P-SSCs were perivascular cells with high osteochondrogenic but minimal adipogenic potential. Upon transplantation into bone injuries in mice, they preserved self-renewal capability in vivo. Single-cell analysis of mouse periosteum further supported the preferential expression of LRP1 and CD13 in Prx1+ P-SSCs. When Lrp1 was conditionally deleted in Prx1 lineage cells, it led to severe bone deformity, short stature, and periosteal defects. By contrast, local treatment with an LRP1 agonist at the injury sites induced early P-SSC proliferation and bone healing. Thus, human and mouse periosteum contains unique osteochondrogenic stem cell subsets, and these P-SSCs express specific markers, LRP1 and CD13, with a regulatory mechanism through LRP1 that enhances P-SSC function and bone repair.

Authors

Youngjae Jeong, Lorenzo Deveza, Laura Ortinau, Kevin Lei, John R. Dawson, Dongsu Park

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Figure 2

Human P-SSCs highly express LRP1, and the combination of LRP1 and SSC markers, CD13+PDPN+PDGFRA+, can specify P-SSC clusters.

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Human P-SSCs highly express LRP1, and the combination of LRP1 and SSC ma...
(A) Heatmaps showing the top 30 DEGs from plasma membrane protein complex in P-SSCs. (B and C) Visualization of periosteal (left) and BM+BM aspirate concentrate (right) cells with UMAP plots showing LRP1 and CD13 gene expression (B) and periosteal surface protein estimation of LRP1 and CD13 expression by SPECK (Surface protein abundance Estimation using CKmeans-based clustered thresholding) method (C). (D) Percentage distribution of LRP1+CD13+PDGFRA+PDPN+ surface protein estimation on each periosteal cluster. (E) LRP1+CD13+PDGFRA+PDPN+ cells on the periosteal cell UMAP plot. (F) FACS analysis of periosteal cell surface expression of LRP1 and PDGFRA in CD13+PDPN+ and CD13PDPN. (G) The surface expression of the indicated SSC markers (CD200, CD105, and CD271) in LRP1+CD13+PDGFRA+PDPN+, CD13PDPN, and whole cells from the periosteum. (HK) Representative immunofluorescence staining images of the indicated markers (CD13, LRP1, and PDPN) on periosteal tissue at 20× (H and I) and 40× (J) original magnification (V, blood vessel). Periosteal cell coexpressing CD13 (green), LRP1 (red), and PDPN (white) are indicated with arrowheads (I), and single-positive cells are indicated with arrow (K).