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Site-Specific Fracture Healing: Comparison between Diaphysis and Metaphysis in the Mouse Long Bone

Journal

Publisher

MDPI
DOI: 10.3390/ijms22179299

Keywords

fracture healing; diaphysis; metaphysis; medullary callus; bone remodeling; estrogen; ovariectomy; Hox genes; skeletal stem cells

Funding

  1. JSPS KAKENHI [20K19546]
  2. Grants-in-Aid for Scientific Research [20K19546] Funding Source: KAKEN

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Fracture healing process varies depending upon internal and external factors, with different fracture sites showing different healing mechanisms. Ovariectomized mice exhibit differences in bone healing after fracture, with estrogen administration affecting diaphyseal healing but not metaphyseal healing. Hox genes play a role in regulating osteoblast differentiation and bone graft adaptability, contributing to the site-specificity of fracture healing.
The process of fracture healing varies depending upon internal and external factors, such as the fracture site, mode of injury, and mechanical environment. This review focuses on site-specific fracture healing, particularly diaphyseal and metaphyseal healing in mouse long bones. Diaphyseal fractures heal by forming the periosteal and medullary callus, whereas metaphyseal fractures heal by forming the medullary callus. Bone healing in ovariectomized mice is accompanied by a decrease in the medullary callus formation both in the diaphysis and metaphysis. Administration of estrogen after fracture significantly recovers the decrease in diaphyseal healing but fails to recover the metaphyseal healing. Thus, the two bones show different osteogenic potentials after fracture in ovariectomized mice. This difference may be attributed to the heterogeneity of the skeletal stem cells (SSCs)/osteoblast progenitors of the two bones. The Hox genes that specify the patterning of the mammalian skeleton during embryogenesis are upregulated during the diaphyseal healing. Hox genes positively regulate the differentiation of osteoblasts from SSCs in vitro. During bone grafting, the SSCs in the donor's bone express Hox with adaptability in the heterologous bone. These novel functions of the Hox genes are discussed herein with reference to the site-specificity of fracture healing.

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