| Literature DB >> 28716575 |
Shailesh Agarwal1, Shawn J Loder1, Christopher Breuler1, John Li1, David Cholok1, Cameron Brownley1, Jonathan Peterson1, Hsiao H Hsieh1, James Drake1, Kavitha Ranganathan1, Yashar S Niknafs1, Wenzhong Xiao2, Shuli Li1, Ravindra Kumar3, Ronald Tompkins4, Michael T Longaker5, Thomas A Davis6, Paul B Yu7, Yuji Mishina8, Benjamin Levi9.
Abstract
Trauma-induced heterotopic ossification (tHO) is a condition of pathologic wound healing, defined by the progressive formation of ectopic bone in soft tissue following severe burns or trauma. Because previous studies have shown that genetic variants of HO, such as fibrodysplasia ossificans progressiva (FOP), are caused by hyperactivating mutations of the type I bone morphogenetic protein receptor (T1-BMPR) ACVR1/ALK2, studies evaluating therapies for HO have been directed primarily toward drugs for this specific receptor. However, patients with tHO do not carry known T1-BMPR mutations. Here we show that, although BMP signaling is required for tHO, no single T1-BMPR (ACVR1/ALK2, BMPR1a/ALK3, or BMPR1b/ALK6) alone is necessary for this disease, suggesting that these receptors have functional redundancy in the setting of tHO. By utilizing two different classes of BMP signaling inhibitors, we developed a translational approach to treatment, integrating treatment choice with existing diagnostic options. Our treatment paradigm balances either immediate therapy with reduced risk for adverse effects (Alk3-Fc) or delayed therapy with improved patient selection but greater risk for adverse effects (LDN-212854).Entities:
Keywords: BMP receptors; BMP signaling; stem cells
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Year: 2017 PMID: 28716575 PMCID: PMC5542633 DOI: 10.1016/j.ymthe.2017.01.008
Source DB: PubMed Journal: Mol Ther ISSN: 1525-0016 Impact factor: 11.454