Thus local or circulating MSC could be target cells for RARγ agon

Thus local or circulating MSC could be target cells for RARγ agonists. Characterization of the effects of RARγ agonist in MSC yielded additional interesting information that could lead to a novel therapeutic strategy. Fig. 3 shows the effect of RARγ agonist pretreatment on the behavior of BMSC in mice. In this experiment,

we first treated BMSC with selective RARγ agonist or vehicle for three days, mixed in Matrigel together with recombinant human BMP-2 and then injected Veliparib in vitro into nude mice. Vehicle treated BMSC remarkably enhanced BMP-2 induced ectopic bone formation in Matrigel (Fig. 3A, upper left) [58]. In contrast, RARγ agonist treated BMSC did not enhance or even decreased BMP-2 induced bone formation. Such trend was consistent in at least three different BMSCs (Fig. http://www.selleckchem.com/products/dinaciclib-sch727965.html 3A, bottom) [58]. In addition, BMSC pretreated with RARγ agonist equally or more effectively facilitated skeletal muscle injury compared to vehicle-treated mice. Those observations suggest

that (1) relatively short term treatment of RARγ agonist can effectively suppress HO for a prolonged time period (2) pretreated MSC may be useful for tissue repair as well as prevention of HO. For example, RARγ agonist pretreated MSC may be effective in preventing the recurrence of HO after surgically removing mature HO. In a dental clinic, we sometimes encounter pathological calcification in a variety of maxillofacial tissues, such as dental ankylosis [60], myositis ossificans in masticatory muscles [61], [62] and [63], and synovial chondromatosis in the temporomandibular joint (TMJ)

[64]. In case of deciduous dentition, removal of the ankylosed tooth is occasionally necessary to prevent click here distorted jaw growth, adverse tooth eruption and space loss [60]. Myositis ossificans is a relatively rare condition characterized by bone neoformation in extraskeletal sites. Like posttraumatic HO, repeated trauma, radiotherapy, long-time intubation with immobilization and critical myopathy and neuropathy are thought to trigger myositis ossificans. The incidence of myositis ossificans in head and neck lesion seems less common compared to those in the extremities [65]. The majority of calcified bodies formed by myositis ossificans are first detected in routine X-ray imaging. Those asymptomatic ectopic bone can be left untreated or removed by surgery. In more severe cases however the ectopic bone could cause limitation in jaw opening, trismus and lead to poor mouth hygiene. Another rare condition is synovial chondromatosis in TMJ. The synovium grows abnormally and produces cartilage nodules [64]. These nodules may break off from the synovium and become loose inside the TMJ and cause severe pain. Surgical removal is the first treatment option. When the sizes of cartilage nodules are small, arthroscopic surgery might be possible.

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