# CD47 is Required for Mesenchymal Progenitor Proliferation and Fracture Repair

**Authors:** Kurt Hankenson, Robert Zondervan, Christina Capobianco, Daniel Jenkins, John Reicha, Livia Frederick, Charles Lam, Jeffery Isenberg, Jaimo Ahn, Ralph S. Marcucio

PMC · DOI: 10.21203/rs.3.rs-4022423/v1 · Research Square · 2024-03-19

## TL;DR

CD47 is important for bone healing, as its absence reduces mesenchymal stem cell proliferation and impairs fracture repair in mice.

## Contribution

This study reveals CD47's novel role in mesenchymal progenitor proliferation and fracture repair in both non-ischemic and ischemic conditions.

## Key findings

- CD47-null mice showed reduced callus bone volume and mineral content after fractures.
- CD47-null mesenchymal stem cells had decreased proliferation and fibroblast colony formation.
- Blocking CD47 in wild-type mice replicated the impaired fracture healing seen in CD47-null mice.

## Abstract

CD47 is a ubiquitous and pleiotropic cell-surface receptor. Disrupting CD47 enhances injury repair in various tissues but the role of CD47 has not been studied in bone injuries. In a murine closed-fracture model, CD47-null mice showed decreased callus bone volume, bone mineral content, and tissue mineral content as assessed by microcomputed tomography 10 days post-fracture, and increased fibrous volume as determined by histology. To understand the cellular basis for this phenotype, mesenchymal progenitors (MSC) were harvested from bone marrow. CD47-null MSC showed decreased large fibroblast colony formation (CFU-F), significantly less proliferation, and fewer cells in S-phase, although osteoblast differentiation was unaffected. However, consistent with prior research, CD47-null endothelial cells showed increased proliferation relative to WT cells. Similarly, in a murine ischemic fracture model, CD47-null mice showed reduced fracture callus bone volume and bone mineral content relative to WT. Consistent with our In vitro results, in vivo EdU labeling showed decreased cell proliferation in the callus of CD47-null mice, while staining for CD31 and endomucin demonstrated increased endothelial cell mass. Finally, WT mice administered a CD47 morpholino, which blocks CD47 protein production, showed a callus phenotype similar to that of non-ischemic and ischemic fractures in CD47-null mice, suggesting the phenotype was not due to developmental changes in the knockout mice. Thus, inhibition of CD47 during bone healing reduces both non-ischemic and ischemic fracture healing, in part, by decreasing MSC proliferation. Furthermore, the increase in endothelial cell proliferation and early blood vessel density caused by CD47 disruption is not sufficient to overcome MSC dysfunction.

## Linked entities

- **Genes:** CD47 (CD47 molecule) [NCBI Gene 961]
- **Proteins:** CD47 (CD47 molecule)
- **Species:** Mus musculus (taxon 10090)

## Full-text entities

- **Genes:** Pecam1 (platelet/endothelial cell adhesion molecule 1) [NCBI Gene 18613] {aka Cd31, PECAM-1, Pecam}, Emcn (endomucin) [NCBI Gene 59308] {aka 0610012K22Rik, Muc14}, Cd47 (CD47 antigen (Rh-related antigen, integrin-associated signal transducer)) [NCBI Gene 16423] {aka 9130415E20Rik, B430305P08Rik, IAP, Itgp}
- **Diseases:** Fracture (MESH:D050723), bone injuries (MESH:D001847), ischemic (MESH:D002545)
- **Species:** Mus musculus (house mouse, species) [taxon 10090]

## Full text

_Full body text omitted from this summary view._ Fetch the complete paper as Markdown: https://tomesphere.com/paper/PMC10984034/full.md

## Figures

9 figures with captions in the complete paper: https://tomesphere.com/paper/PMC10984034/full.md

## References

50 references — full list in the complete paper: https://tomesphere.com/paper/PMC10984034/full.md

---
Source: https://tomesphere.com/paper/PMC10984034