TY - JOUR
T1 - Heterotopic ossifcation has some nerve
AU - Salisbury, Elizabeth
AU - Sonnet, Corinne
AU - Heggeness, Michael
AU - Davis, Alan R.
AU - Olmsted-Davis, Elizabeth
PY - 2010
Y1 - 2010
N2 - Heterotopic ossifcation, defned as the formation of bone in abnormal anatomic locations, can be clinically insignifcant or devastating and debilitating, depending on the site and duration of new bone formation. Tere are many causes of heterotopic ossifcation (HO), including soft tissue trauma, central nervous system injury, vasculopathies, arthropathies, and inheritance. One of the least understood components of HO is the interaction of the peripheral nervous system with the induction of this process. Recent work has shown that, upon traumatic injury, a cascade of events termed neurogenic infammation is initiated, which involves the release of neuropeptides, such as substance P and calcitonin gene related peptide. Release of these peptides ultimately leads to the recruitment of activated platelets, mast cells, and neutrophils to the injury site. Tese cells appear to be involved with both remodeling of the nerve, as well as potentially recruiting additional cells from the bone marrow to the injury site. Further, sensory neurons stimulated at the injury site relay local information to the brain, which can then redirect neuroendocrine signaling in the hypothalamus towards repair of the injured site. While numerous studies have highlighted the important role of nerve-derived signals, both central and peripheral, in the regulation of normal bone remodeling of the skeleton,1 this review focuses on the role of the local, peripheral nerves in the formation of heterotopic bone. We concentrate on the manner in which local changes in bone morphogenetic protein (BMP) expression contribute to a cascade of events within the peripheral nerves, both sensory and sympathetic, in the immediate area of HO formation.
AB - Heterotopic ossifcation, defned as the formation of bone in abnormal anatomic locations, can be clinically insignifcant or devastating and debilitating, depending on the site and duration of new bone formation. Tere are many causes of heterotopic ossifcation (HO), including soft tissue trauma, central nervous system injury, vasculopathies, arthropathies, and inheritance. One of the least understood components of HO is the interaction of the peripheral nervous system with the induction of this process. Recent work has shown that, upon traumatic injury, a cascade of events termed neurogenic infammation is initiated, which involves the release of neuropeptides, such as substance P and calcitonin gene related peptide. Release of these peptides ultimately leads to the recruitment of activated platelets, mast cells, and neutrophils to the injury site. Tese cells appear to be involved with both remodeling of the nerve, as well as potentially recruiting additional cells from the bone marrow to the injury site. Further, sensory neurons stimulated at the injury site relay local information to the brain, which can then redirect neuroendocrine signaling in the hypothalamus towards repair of the injured site. While numerous studies have highlighted the important role of nerve-derived signals, both central and peripheral, in the regulation of normal bone remodeling of the skeleton,1 this review focuses on the role of the local, peripheral nerves in the formation of heterotopic bone. We concentrate on the manner in which local changes in bone morphogenetic protein (BMP) expression contribute to a cascade of events within the peripheral nerves, both sensory and sympathetic, in the immediate area of HO formation.
KW - BMP2
KW - Heterotopic ossifcation
KW - Neurogenic infammation
KW - Peripheral nervous system
KW - Sensory
KW - Sympathetic
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U2 - 10.1615/CritRevEukarGeneExpr.v20.i4.30
DO - 10.1615/CritRevEukarGeneExpr.v20.i4.30
M3 - Article
C2 - 21395504
AN - SCOPUS:79954994746
SN - 1045-4403
VL - 20
SP - 313
EP - 324
JO - Critical Reviews in Eukaryotic Gene Expression
JF - Critical Reviews in Eukaryotic Gene Expression
IS - 4
ER -