Quiescent Bone Lining Cells Are a Major Source of Osteoblasts During Adulthood

Author:

Matic Igor1,Matthews Brya G.1,Wang Xi1,Dyment Nathaniel A.1,Worthley Daniel L.2,Rowe David W.1,Grcevic Danka3,Kalajzic Ivo1

Affiliation:

1. Department of Reconstructive Sciences, University of Connecticut Health Center, Farmington, Connecticut, USA

2. Department of Medicine and Cancer Theme, University of Adelaide & SAHMRI, Adelaide, South Australia, Australia

3. Department of Physiology and Immunology, School of Medicine, University of Zagreb, Zagreb, Croatia

Abstract

Abstract The in vivo origin of bone-producing osteoblasts is not fully defined. Skeletal stem cells, a population of mesenchymal stem cells resident in the bone marrow compartment, are thought to act as osteoprogenitors during growth and adulthood. Quiescent bone lining cells (BLCs) have been suggested as a population capable of activation into mature osteoblasts. These cells were defined by location and their morphology and studies addressing their significance have been hampered by their inaccessibility, and lack of markers that would allow for their identification and tracing. Using lineage tracing models, we have observed labeled osteoblasts at time points extending beyond the reported lifespan for this cell type, suggesting continuous reactivation of BLCs. BLCs also make a major contribution to bone formation after osteoblast ablation, which includes the ability to proliferate. In contrast, mesenchymal progenitors labeled by Gremlin1 or alpha smooth muscle actin do not contribute to bone formation in this setting. BLC activation is inhibited by glucocorticoids, which represent a well-established cause of osteoporosis. BLCs express cell surface markers characteristic of mesenchymal stem/progenitors that are largely absent in osteoblasts including Sca1 and Leptin Receptor. BLCs also show different gene expression profiles to osteoblasts, including elevated expression of Mmp13, and osteoclast regulators RANKL and macrophage colony stimulating factor, and retain osteogenic potential upon transplantation. Our findings provide evidence that bone lining cells represent a major source of osteoblasts during adulthood.

Funder

NIH/NIAMS

Connecticut Regenerative Medicine Research Fund

NIH/NIDCR

Publisher

Oxford University Press (OUP)

Subject

Cell Biology,Developmental Biology,Molecular Medicine

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