Excess BMP Signaling in Heterotopic Cartilage Forming in <i>Prg4</i>-null TMJ Discs

Bechtold, Till Edward; Saunders, Cheri; Mundy, Christina; Um, H.; Decker, Rebekah S.; Salhab, Imad; Kurio, Naito; Billings, Paul C.; Pacifici, Maurizio; Nah, Hyun-Duck; Koyama, Eiki

doi:10.1177/0022034515613508

Cited by 17 publications

(23 citation statements)

References 44 publications

(51 reference statements)

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“…Cultures were prepared from glenoid fossa/eminence samples isolated from 2 month-old wild-type mice (n=32) as described (Bechtold et al, 2015) with some modifications. Isolated glenoid fossae were incubated with 2.5 U/ml dispase (MP Biomedicals, LLC, Solon, OH) and 600 U/ml (3mg/ml) type I collagenase (Worthington Biochemical Corporation, Lakewood, NJ) in HBSS with Ca 2+ and Mg 2+ for 10 min at 37°C with agitation, and then the surface was curetted.…”

Section: Methodsmentioning

confidence: 99%

“…(Hill et al, 2014; Koyama et al, 2014). We also reported that Prg4 -null mice displayed increased levels of chondrogenesis and ectopic cartilage formation within TMJ components (Bechtold et al, 2015; Koyama et al, 2014), but the cellular, signaling and molecular mechanisms underling such potentially important pathogenic transformation remains unclear.…”

Section: Introductionmentioning

confidence: 99%

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Osteophyte formation and matrix mineralization in a TMJ osteoarthritis mouse model are associated with ectopic hedgehog signaling

et al. 2016

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The temporomandibular joint (TMJ) is a diarthrodial joint that relies on lubricants for frictionless movement and long-term function. It remains unclear what temporal and causal relationships may exist between compromised lubrication and onset and progression of TMJ disease. Here we report that Proteoglycan 4 (Prg4)-null TMJs exhibit irreversible osteoarthritis-like changes over time and are linked to formation of ectopic mineralized tissues and osteophytes in articular disc, mandibular condyle and glenoid fossa. In the presumptive layer of mutant glenoid fossa’s articulating surface, numerous chondrogenic cells and/or chondrocytes emerged ectopically within the type I collagen-expressing cell population, underwent endochondral bone formation accompanied by enhanced Ihh expression, became entrapped into temporal bone mineralized matrix, and thereby elicited excessive chondroid bone formation. As the osteophytes grew, the roof of the glenoid fossa/eminence became significantly thicker and flatter, resulting in loss of its characteristic concave shape for accommodation of condyle and disc. Concurrently, the condyles became flatter and larger and exhibited ectopic bone along their neck, likely supporting the enlarged condylar heads. Articular discs lost their concave configuration, and ectopic cartilage developed and articulated with osteophytes. In glenoid fossa cells in culture, hedgehog signaling stimulated chondrocyte maturation and mineralization including alkaline phosphatase, while treatment with hedgehog inhibitor HhAntag prevented such maturation process. In sum, our data indicate that Prg4 is needed for TMJ integrity and long-term postnatal function. In its absence, progenitor cells near presumptive articular layer and disc undergo ectopic chondrogenesis and generate ectopic cartilage, possibly driven by aberrant activation of Hh signaling. The data suggest also that the Prg4-null mice represent a useful model to study TMJ osteoarthritis-like degeneration and clarify its pathogenesis.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Osteophyte formation and matrix mineralization in a TMJ osteoarthritis mouse model are associated with ectopic hedgehog signaling

et al. 2016

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“…Results from this study illustrate that BMP-2 treatment potentiated the induction of Acan, Col2 , Col 10 , and Ihh in Bgn −/− Fmod −/− mice. Excess BMP-2 signaling has also been implicated in the pathogenesis of accelerated TMJ-OA in Pgr4-KO mice [Bechtold et al 2016]. In contrast, absence of BMP signaling in transgenic mice with Bmp1Ra conditionally deleted in neural crest cells led to failure of articular disc separation from the hypoplastic condyle and under development of the mandibular condylar cartilage [Gu et al 2014].…”

Section: Discussionmentioning

confidence: 99%

“…Abnormal activation of this signaling causes heterotopic cartilage and bone formation [Huegel et al 2015, Billings et al, 2008]. Specifically, excessive BMP-2 signaling has recently been shown to be involved in heterotopic cartilage formation and the pathogenesis of TMJ-OA [Bechtold et al 2016, Albilia et al, 2013]. However, the mechanism of excessive BMP-2 signaling on the mandibular condylar cartilage and its implications in TMJ-OA are unknown.…”

Section: Introductionmentioning

confidence: 99%

Extracellular Matrix Mediates BMP-2 in a Model of Temporomandibular Joint Osteoarthritis

Shirakura

Kram

Robinson

et al. 2017

Cells Tissues Organs

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Temporomandibular joint (TMJ) osteoarthritis (OA) is a complex disease that affects both cartilage and subchondral bone. It is accompanied by loss of extracellular matrix (ECM) and may be controlled by bone morphogenetic protein-2 (BMP-2). We analyzed the effect of BMP-2 in both cartilage and subchondral bone in a TMJ-OA animal model that is deficient in biglycan (Bgn) and fibromodulin (Fmod) (Bgn^-/-Fmod^-/-). Whole mandibles were dissected from 3-week-old wild-type (WT) and Bgn^-/-Fmod^-/- mice and incubated with and without 250 µg/mL BMP-2 for 2 days using an explant culture system. Condyle growth was measured by microCT and the expression levels of cartilage and bone-related genes were analyzed using RT-PCR or by immunohistochemistry from condyles that contained an intact cartilage/subchondral bone interface. Osteoclast activity was estimated by tartrate-resistant acid phosphatase (TRAP) staining and by TRAP, Rankl, and Adamts4 mRNA expression levels. Our results showed that most parameters examined were slightly up-regulated in WT samples treated with BMP-2, and this up-regulation was significantly enhanced in the Bgn^-/-Fmod^-/- mice. The up-regulation of both catabolic and anabolic agents did not appear to positively affect the overall growth of Bgn^-/-Fmod^-/- condyles compared to WT controls. In summary, the up-regulation of both anabolic and catabolic genes in the WT and Bgn^-/-Fmod^-/- TMJs treated with BMP-2 suggests that BMP increases matrix turnover in the condyle, and, further, that Bgn and Fmod could have protective roles in regulating this process.

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“…In seeking for effective treatment and functional repair strategies, murine model becomes a necessary and unique in vivo platform, as its availability for genetic modification and short lifespan enable pinpointing the TMJ development, biology and pathogenesis to specific molecules or signaling pathways (Suzuki and Iwata, 2016). Evaluation of the phenotype in genetically modified mice has provided new insights into the roles of individual matrix molecules in TMJ development and OA, such as lubricin (Bechtold et al, 2016; Hill et al, 2014; Koyama et al, 2014), biglycan and fibromodulin (Wadhwa et al, 2005), collagen types II (Ricks et al, 2013) and XI (Xu et al, 2003). In addition, aided by clinically relevant operations such as partial discectomy (Xu et al, 2009) and anterior crossbite prosthesis (Liu et al, 2014), TMJ OA can be induced in mice to study the disease initiation and progression in a well-defined timeframe in vivo.…”

Section: Introductionmentioning

confidence: 99%

Biomechanical properties of murine TMJ articular disc and condyle cartilage via AFM-nanoindentation

Chandrasekaran

Doyran

et al. 2017

Journal of Biomechanics

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This study aims to quantify the biomechanical properties of murine temporomandibular joint (TMJ) articular disc and condyle cartilage using AFM-nanoindentation. For skeletally mature, 3-month old mice, the surface of condyle cartilage was found to be significantly stiffer (306 ± 84 kPa, mean ± 95% CI) than those of the superior (85 ± 23 kPa) and inferior (45 ± 12 kPa) sides of the articular disc. On the disc surface, significant heterogeneity was also detected across multiple anatomical sites, with the posterior end being the stiffest and central region being the softest. Using SEM, this study also found that the surfaces of disc are composed of anteroposteriorly oriented collagen fibers, which are sporadically covered by thinner random fibrils. Such fibrous nature results in both an F-D3/2 indentation response, which is a typical Hertzian response for soft continuum tissue under a spherical tip, and a linear F-D response, which is typical for fibrous tissues, further signifying the high degree of tissue heterogeneity. In comparison, the surface of condyle cartilage is dominated by thinner, randomly oriented collagen fibrils, leading to Hertzian-dominated indentation responses. As the first biomechanical study of murine TMJ, this work will provide a basis for future investigations of TMJ tissue development and osteoarthritis in various murine TMJ models.

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Excess BMP Signaling in Heterotopic Cartilage Forming in Prg4-null TMJ Discs

Cited by 17 publications

References 44 publications

Osteophyte formation and matrix mineralization in a TMJ osteoarthritis mouse model are associated with ectopic hedgehog signaling

Osteophyte formation and matrix mineralization in a TMJ osteoarthritis mouse model are associated with ectopic hedgehog signaling

Extracellular Matrix Mediates BMP-2 in a Model of Temporomandibular Joint Osteoarthritis

Biomechanical properties of murine TMJ articular disc and condyle cartilage via AFM-nanoindentation

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