TY - JOUR
T1 - Targeted stimulation of retinoic acid receptor-γ mitigates the formation of heterotopic ossification in an established blast-related traumatic injury model
AU - Pavey, Gabriel J.
AU - Qureshi, Ammar T.
AU - Tomasino, Allison M.
AU - Honnold, Cary L.
AU - Bishop, Danett K.
AU - Agarwal, Shailesh
AU - Loder, Shawn
AU - Levi, Benjamin
AU - Pacifici, Maurizio
AU - Iwamoto, Masahiro
AU - Potter, Benjamin K.
AU - Davis, Thomas A.
AU - Forsberg, Jonathan A.
N1 - Funding Information:
We like to thank Dr. Matthew Wagner, Dr. John Tra and Mr. Ying Cao for their assistance with statistical analysis. This work was supported by CDMRP grant W81XWH-13-2-0077 (to JAF) and grant H81XWH-13-2-0076 (to MP). B.L. received funding from NIH/NIGMS - K08GM109105-0, Plastic Surgery Foundation National Endowment Award, the Association for Academic Surgery Roslyn Award American Association for the Surgery of Trauma Research & Education Foundation Scholarship, and American Association of Plastic Surgery Research Fellowship. SJL funded by a Howard Hughes Medical Institute research fellowship. SA funded by the NIH LRP, Coller Society, and Plastic Surgery Foundation.
Publisher Copyright:
© 2016
PY - 2016/9/1
Y1 - 2016/9/1
N2 - Heterotopic ossification (HO) involves formation of endochondral bone at non-skeletal sites, is prevalent in severely wounded service members, and causes significant complications and delayed rehabilitation. As common prophylactic treatments such as anti-inflammatory drugs and irradiation cannot be used after multi-system combat trauma, there is an urgent need for new remedies. Previously, we showed that the retinoic acid receptor γ agonist Palovarotene inhibited subcutaneous and intramuscular HO in mice, but those models do not mimic complex combat injury. Thus, we tested Palovarotene in our validated rat trauma-induced HO model that involves blast-related limb injury, femoral fracture, quadriceps crush injury, amputation and infection with methicillin-resistant Staphylococcus aureus from combat wound infections. Palovarotene was given orally for 14 days at 1 mg/kg/day starting on post-operative day (POD) 1 or POD-5, and HO amount, wound dehiscence and related processes were monitored for up to 84 days post injury. Compared to vehicle-control animals, Palovarotene significantly decreased HO by 50 to 60% regardless of when the treatment started and if infection was present. Histological analyses showed that Palovarotene reduced ectopic chondrogenesis, osteogenesis and angiogenesis forming at the injury site over time, while fibrotic tissue was often present in place of ectopic bone. Custom gene array data verified that while expression of key chondrogenic and osteogenic genes was decreased within soft tissues of residual limb in Palovarotene-treated rats, expression of cartilage catabolic genes was increased, including matrix metalloproteinase-9. Importantly, Palovarotene seemed to exert moderate inhibitory effects on wound healing, raising potential safety concerns related to dosing and timing. Our data show for the first time that Palovarotene significantly inhibits HO triggered by blast injury and associated complications, strongly indicating that it may prevent HO in patients at high risk such as those sustaining combat injuries and other forms of blast trauma.
AB - Heterotopic ossification (HO) involves formation of endochondral bone at non-skeletal sites, is prevalent in severely wounded service members, and causes significant complications and delayed rehabilitation. As common prophylactic treatments such as anti-inflammatory drugs and irradiation cannot be used after multi-system combat trauma, there is an urgent need for new remedies. Previously, we showed that the retinoic acid receptor γ agonist Palovarotene inhibited subcutaneous and intramuscular HO in mice, but those models do not mimic complex combat injury. Thus, we tested Palovarotene in our validated rat trauma-induced HO model that involves blast-related limb injury, femoral fracture, quadriceps crush injury, amputation and infection with methicillin-resistant Staphylococcus aureus from combat wound infections. Palovarotene was given orally for 14 days at 1 mg/kg/day starting on post-operative day (POD) 1 or POD-5, and HO amount, wound dehiscence and related processes were monitored for up to 84 days post injury. Compared to vehicle-control animals, Palovarotene significantly decreased HO by 50 to 60% regardless of when the treatment started and if infection was present. Histological analyses showed that Palovarotene reduced ectopic chondrogenesis, osteogenesis and angiogenesis forming at the injury site over time, while fibrotic tissue was often present in place of ectopic bone. Custom gene array data verified that while expression of key chondrogenic and osteogenic genes was decreased within soft tissues of residual limb in Palovarotene-treated rats, expression of cartilage catabolic genes was increased, including matrix metalloproteinase-9. Importantly, Palovarotene seemed to exert moderate inhibitory effects on wound healing, raising potential safety concerns related to dosing and timing. Our data show for the first time that Palovarotene significantly inhibits HO triggered by blast injury and associated complications, strongly indicating that it may prevent HO in patients at high risk such as those sustaining combat injuries and other forms of blast trauma.
KW - Animal model
KW - Bioburden
KW - Blast overpressure exposure
KW - Endochondral ossification
KW - Heterotopic ossification
KW - Prophylaxis
KW - Retinoic acid receptor-γ agonist
KW - Traumatic extremity injury
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U2 - 10.1016/j.bone.2016.06.014
DO - 10.1016/j.bone.2016.06.014
M3 - Article
C2 - 27368930
AN - SCOPUS:84976870625
SN - 8756-3282
VL - 90
SP - 159
EP - 167
JO - Bone
JF - Bone
ER -