Lienau
J, Schell H, Epari DR, Schütze N*, Jakob F*, Bail HJ, Duda GN
Center for Musculoskeletal
Surgery, Charité – Universitätsmedizin Berlin,
Free and Humboldt-University of Berlin, Germany
*Clinical Research Group on Musculoskeletal Diseases, Orthopaedic Department,
University of Würzburg, Germany
The formation of new blood vessels is a prerequisite for bone healing.
CYR61 (CCN1), an extracellular matrix-associated signaling protein,
is a potent stimulator of angiogenesis and mesenchymal stem cell expansion
and differentiation. A recent study showed that CYR61 is expressed during
fracture healing and suggested that CYR61 plays a significant role in
cartilage and bone formation. The hypothesis of the present study was
that decreased fixation stability, which leads to a delay in healing,
would lead to reduced CYR61 protein expression in fracture callus. The
aim of the study was to quantitatively analyze CYR61 protein expression,
vascularization and tissue differentiation in the osteotomy gap and
relate to the mechanical fixation stability during the course of healing.
A mid-shaft osteotomy of the tibia was performed in two groups of sheep
and stabilized with either a rigid or semirigid external fixator, each
allowing different amounts of interfragmentary movement. The sheep were
sacrificed at 2, 3, 6, and 9 weeks postoperatively. The tibiae were
tested biomechanically and histological sections from the callus were
analyzed immunohistochemically with regard to CYR61 protein expression
and vascularization. Expression of CYR61 protein was upregulated at
the early phase of fracture healing (2 weeks), decreasing over the healing
time. Decreased fixation stability was associated with a reduced upregulation
of the CYR61 protein expression and a reduced vascularization at 2 weeks
leading to a slower healing. The maximum cartilage callus fraction in
both groups was reached at 3 weeks. However, the semirigid fixator group
showed a significantly lower CYR61 immunoreactivity in cartilage than
the rigid fixator group at this time point. The fraction of cartilage
in the semirigid fixator group was not replaced by bone as quickly as
in the rigid fixator group leading to an inferior histological and mechanical
callus quality at 6 weeks and therefore to a slower healing. The results
supply further evidence that CYR61 may serve as an important regulator
of bone healing.
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