Literature DB >> 30142335

Characterizing the Circulating Cell Populations in Traumatic Heterotopic Ossification.

Shawn J Loder1, Shailesh Agarwal1, Michael T Chung1, David Cholok1, Charles Hwang1, Noelle Visser1, Kaetlin Vasquez1, Michael Sorkin1, Joe Habbouche1, Hsiao H Sung1, Joshua Peterson1, David Fireman1, Kavitha Ranganathan1, Christopher Breuler1, Caitlin Priest1, John Li1, Xue Bai1, Shuli Li1, Paul S Cederna1, Benjamin Levi2.   

Abstract

Heterotopic ossification (HO) occurs secondary to trauma, causing pain and functional limitations. Identification of the cells that contribute to HO is critical to the development of therapies. Given that innate immune cells and mesenchymal stem cells are known contributors to HO, we sought to define the contribution of these populations to HO and to identify what, if any, contribution circulating populations have to HO. A shared circulation was obtained using a parabiosis model, established between an enhanced green fluorescent protein-positive/luciferase+ donor and a same-strain nonreporter recipient mouse. The nonreporter mouse received Achilles tendon transection and dorsal burn injury to induce HO formation. Bioluminescence imaging and immunostaining were performed to define the circulatory contribution of immune and mesenchymal cell populations. Histologic analysis showed circulating cells present throughout each stage of the developing HO anlagen. Circulating cells were present at the injury site during the inflammatory phase and proliferative period, with diminished contribution in mature HO. Immunostaining demonstrated that most early circulatory cells were from the innate immune system; only a small population of mesenchymal cells were present in the HO. We demonstrate the time course of the participation of circulatory cells in trauma-induced HO and identify populations of circulating cells present in different stages of HO. These findings further elucidate the relative contribution of local and systemic cell populations to HO.
Copyright © 2018 American Society for Investigative Pathology. Published by Elsevier Inc. All rights reserved.

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Year:  2018        PMID: 30142335      PMCID: PMC6222270          DOI: 10.1016/j.ajpath.2018.07.014

Source DB:  PubMed          Journal:  Am J Pathol        ISSN: 0002-9440            Impact factor:   4.307


  38 in total

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