Loss of Smad4 in the scleraxis cell lineage results in postnatal joint contracture

Loss of Smad4 in the scleraxis cell lineage results in postnatal joint contracture

Growth of the musculoskeletal system requires precise coordination between bone, muscle, and tendon during development. Insufficient elongation of the muscle-tendon unit relative to bone growth results in joint contracture, a condition characterized by reduction or complete loss of joint range of mo...

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Veröffentlicht in:Developmental biology 2021-02, Vol.470, p.108-120
Hauptverfasser: Schlesinger, Saundra Y., Seo, Seongkyung, Pryce, Brian A., Tufa, Sara F., Keene, Douglas R., Huang, Alice H., Schweitzer, Ronen
Format: Artikel
Sprache:eng
Schlagworte:
Animals
BMP
Bone Development
Bone Morphogenetic Proteins - metabolism
Cartilage - growth & development
Cartilage - metabolism
Cell Lineage
Collagen - metabolism
Contracture - metabolism
Contracture - pathology
Extracellular Matrix - metabolism
Forelimb
Joint contracture
Mice
Muscle, Skeletal - metabolism
Signal Transduction
Smad4
Smad4 Protein - genetics
Smad4 Protein - metabolism
Tendon
Tendons - cytology
Tendons - embryology
Tendons - growth & development
Tendons - metabolism
TGFβ
Transforming Growth Factor beta - metabolism
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Zusammenfassung:Growth of the musculoskeletal system requires precise coordination between bone, muscle, and tendon during development. Insufficient elongation of the muscle-tendon unit relative to bone growth results in joint contracture, a condition characterized by reduction or complete loss of joint range of motion. Here we establish a novel murine model of joint contracture by targeting Smad4 for deletion in the tendon cell lineage using Scleraxis-Cre (ScxCre). Smad4ScxCre mutants develop a joint contracture shortly after birth. The contracture is stochastic in direction and increases in severity with age. Smad4ScxCre mutant tendons exhibited a stable reduction in cellularity and a progressive reduction in extracellular matrix volume. Collagen fibril diameters were reduced in the Smad4ScxCre mutants, suggesting a role for Smad4 signaling in the regulation of matrix accumulation. Although ScxCre also has sporadic activity in both cartilage and muscle, we demonstrate an essential role for Smad4 loss in tendons for the development of joint contractures. Disrupting the canonical TGFβ-pathway in Smad2;3ScxCre mutants did not result in joint contractures. Conversely, disrupting the BMP pathway by targeting BMP receptors (Alk3ScxCre/Alk6null) recapitulated many features of the Smad4ScxCre contracture phenotype, suggesting that joint contracture in Smad4ScxCre mutants is caused by disruption of BMP signaling. Overall, these results establish a model of murine postnatal joint contracture and a role for BMP signaling in tendon elongation and extracellular matrix accumulation. •Targeting the Smad4 gene in the tendon cell lineage leads to postnatal joint contracture.•The Smad4 contracture phenotype reflects an essential role for BMP signaling in regulation of tendon growth.•Smad4 mutant tendons are thinner with fewer tenocytes and lacking very large collagen fibrils.•Postnatal targeting of Smad4 in tenocytes results in reduced collagen fibril diameters but no joint contracture.
ISSN:0012-1606
1095-564X
DOI:10.1016/j.ydbio.2020.11.006