Apyrase as a novel therapeutic inhibitor of heterotopic ossification
Heterotopic ossification (HO) is a disabling disorder where endochondral bone forms in soft tissue (1). Genetic diseases, traumatic injuries, or severe burns can induce this pathological condition and can lead to severe immobility (2). While the mechanisms by which the bony lesions arise are not completely understood, intense inflammation associated with musculoskeletal injury and/or highly invasive orthopaedic surgery is thought to induce HO. The incidence of HO has been reported between 3% and 90% following total hip arthoplasty or severe fracture of the long bones (3). While the vast majority of these cases are asymptomatic, some patients will present decreased range of motion and painful swelling around the affected joints leading to severe immobility. In severe cases, ectopic bone formation may be involved in implant failure, leading to costly and painful revision surgery (4). Currently, no treatment modalities exist for HO and attempts to prevent the ectopic formation of bone have had only limited success. Early diagnosis of the formation of ectopic bone is complicated by the absence of calcium in the matrix during the first few weeks following surgery, making X-ray detection of ectopic bone very difficult. Prophylactic radiation therapy, anti-inflammatory, and bisphosphonates agents have shown some promise in preventing HO, but their effects are mild to moderate at best and complicated with adverse effects (5). Furthermore, none of these treatment modalities target key signaling pathways critical in the development of the extra skeletal bone tissue formation.
Bone morphogenetic proteins (BMP) such as BMP2, BMP4, and BMP9 have been shown to promote HO when injected into the muscle tissue of mice (6-8) and are highly expressed in human lesions of heterotopic bone (9,10). In individuals suffering from fibrodysplasia ossificans progressiva (FOP), a rare genetic disorder where patients exhibit massive HO and form an ectopic skeleton (2), a single point mutation in the ACVR1 gene causing a change in amino acid 206 (R206H) of the BMP type I receptor activin-like kinase 2 (ALK2) disrupts an α-helix in the glycine-serine rich domain, rendering ALK2 constitutively active (11,12). ALK2 activity causes phosphorylation of Smad proteins (13) and has been shown to regulate endothelial-mesenchymal transition (EndMT) and stem cell differentiation to form new skeletal tissue (7,14).
The discovery of the ALK2 mutation in FOP has provided the most direct therapeutic strategy by inhibiting this BMP receptor. Studies using chemical inhibitors of ALK2 called dorsomorphin and LDN-193189 have been successful in preventing HO in mice (15). A further study showed that the BMP type II receptor is required for HO in mutant ALK2 transgenic mice (16), providing another therapeutic target.
Other studies have shown that mice with defective sensory neurons show impaired BMP-induced HO (17). A neuropeptide released by sensory neurons called Substance P, which causes recruitment and degranulation of mast cells, plays a significant role in HO. RP-67580, a Substance P antagonist, significantly reduces BMP4-induced HO in mice (18). An anti-histamine called Cromolyn, which blocks mast cell degranulation, also significantly reduces HO in mice (17). Interestingly, retinoic acid receptor-γ agonists have been identified to be tremendously effective pharmacological inhibitors of HO by impairing chondrogenesis and endochondral ossification and represent the most promising drugs to date for potential clinical application to prevent HO (19). However, novel therapeutic strategies are needed to avoid potential side effects of such inhibitors.
In a recent issue of Science Translational Medicine, Peterson et al. show that burn injury-induced HO can be treated through a novel therapeutic called apyrase, which causes ATP hydrolysis and modulation of Smad1/5/8 phosphorylation (20). The authors analyzed adipose tissue and adipose-derived mesenchymal stem cells (MSCs) from burn patients and found elevated BMP-dependent Smad signaling and osteogenic differentiation compared to control groups. In a mouse burn model (dorsal scald burn) the injury showed similar increased BMP signaling and osteogenic potential. Addition of the ALK2 inhibitor LDN-193189 decreased the osteogenic potential of MSCs from the burn site. Elevated levels of ATP and decreased levels of cAMP were observed after burn injury (20). cAMP has been described to inhibit Smad1/5/8 phosphorylation (21). The authors used topical apyrase, an ATP hydrolyzing agent, at the burn site and showed that it inhibited BMP signaling and osteogenic differentiation of MSCs, thereby preventing HO at the site of injury. Interestingly, application of apyrase to the burn site also inhibited HO caused by Achilles tenotomy (20). Small molecule therapeutics such as LDN-193189 may result in severe off-target effects thereby impairing their clinical utility in preventing HO (22). However, local application of apyrase at the site of burn or injury may more efficient and effective than other potential HO therapies.
It would be beneficial to test whether apyrase would alleviate HO in an animal model of FOP or in patients afflicted with this debilitating disorder. Clinical studies should also be done to assess the effects of apyrase in patients with various forms of trauma-induced HO. Targeting ATP hydrolysis using apyrase has great potential for clinical application in HO treatment and will likely improve current therapeutic strategies.
Acknowledgements
Funding: This work was supported by grants R01HL112860 (to D Medici), P20GM104937 (to D Medici and AM Reginato), and P20GM103652 (to OD Liang) from the National Institutes of Health and a grant from the John Butler Mulliken Foundation (to D Medici).
Disclosure: The authors declare no conflict of interest.
References
- Shore EM, Kaplan FS. Inherited human diseases of heterotopic bone formation. Nat Rev Rheumatol 2010;6:518-27. [PubMed]
- Kaplan FS, Chakkalakal SA, Shore EM. Fibrodysplasia ossificans progressiva: mechanisms and models of skeletal metamorphosis. Dis Model Mech 2012;5:756-62. [PubMed]
- Board TN, Karva A, Board RE, et al. The prophylaxis and treatment of heterotopic ossification following lower limb arthroplasty. J Bone Joint Surg Br 2007;89:434-40. [PubMed]
- Brenke C, Scharf J, Schmieder K, et al. High prevalence of heterotopic ossification after cervical disc arthroplasty: outcome and intraoperative findings following explantation of 22 cervical disc prostheses. J Neurosurg Spine 2012;17:141-6. [PubMed]
- Baird EO, Kang QK. Prophylaxis of heterotopic ossification - an updated review. J Orthop Surg Res 2009;4:12. [PubMed]
- Lounev VY, Ramachandran R, Wosczyna MN, et al. Identification of progenitor cells that contribute to heterotopic skeletogenesis. J Bone Joint Surg Am 2009;91:652-63. [PubMed]
- Medici D, Shore EM, Lounev VY, et al. Conversion of vascular endothelial cells into multipotent stem-like cells. Nat Med 2010;16:1400-6. [PubMed]
- Leblanc E, Trensz F, Haroun S, et al. BMP-9-induced muscle heterotopic ossification requires changes to the skeletal muscle microenvironment. J Bone Miner Res 2011;26:1166-77. [PubMed]
- Gannon FH, Kaplan FS, Olmsted E, et al. Bone morphogenetic protein 2/4 in early fibromatous lesions of fibrodysplasia ossificans progressiva. Hum Pathol 1997;28:339-43. [PubMed]
- Grenier G, Leblanc E, Faucheux N, et al. BMP-9 expression in human traumatic heterotopic ossification: a case report. Skelet Muscle 2013;3:29. [PubMed]
- Shore EM, Xu M, Feldman GJ, et al. A recurrent mutation in the BMP type I receptor ACVR1 causes inherited and sporadic fibrodysplasia ossificans progressiva. Nat Genet 2006;38:525-7. [PubMed]
- Groppe JC, Shore EM, Kaplan FS. Functional modeling of the ACVR1 (R206H) mutation in FOP. Clin Orthop Relat Res 2007;87-92. [PubMed]
- Miyazono K, Maeda S, Imamura T. BMP receptor signaling: transcriptional targets, regulation of signals, and signaling cross-talk. Cytokine Growth Factor Rev 2005;16:251-63. [PubMed]
- van Dinther M, Visser N, de Gorter DJ, et al. ALK2 R206H mutation linked to fibrodysplasia ossificans progressiva confers constitutive activity to the BMP type I receptor and sensitizes mesenchymal cells to BMP-induced osteoblast differentiation and bone formation. J Bone Miner Res 2010;25:1208-15. [PubMed]
- Yu PB, Deng DY, Lai CS, et al. BMP type I receptor inhibition reduces heterotopic [corrected] ossification. Nat Med 2008;14:1363-9. [PubMed]
- Bagarova J, Vonner AJ, Armstrong KA, et al. Constitutively active ALK2 receptor mutants require type II receptor cooperation. Mol Cell Biol 2013;33:2413-24. [PubMed]
- Salisbury E, Rodenberg E, Sonnet C, et al. Sensory nerve induced inflammation contributes to heterotopic ossification. J Cell Biochem 2011;112:2748-58. [PubMed]
- Kan L, Lounev VY, Pignolo RJ, et al. Substance P signaling mediates BMP-dependent heterotopic ossification. J Cell Biochem 2011;112:2759-72. [PubMed]
- Shimono K, Tung WE, Macolino C, et al. Potent inhibition of heterotopic ossification by nuclear retinoic acid receptor-γ agonists. Nat Med 2011;17:454-60. [PubMed]
- Peterson JR, De La Rosa S, Eboda O, et al. Treatment of heterotopic ossification through remote ATP hydrolysis. Sci Transl Med 2014;6:255ra132.
- Zhang S, Kaplan FS, Shore EM. Different roles of GNAS and cAMP signaling during early and late stages of osteogenic differentiation. Horm Metab Res 2012;44:724-31. [PubMed]
- Sanvitale CE, Kerr G, Chaikuad A, et al. A new class of small molecule inhibitor of BMP signaling. PLoS One 2013;8:e62721. [PubMed]