4.7 Article

Molecular Mechanisms of Fetal Tendon Regeneration Versus Adult Fibrous Repair

期刊

出版社

MDPI
DOI: 10.3390/ijms22115619

关键词

tendon healing; regeneration; inflammation; tendinopathy; proteomics; animal model; fetal

资金

  1. Austrian Agency for International Cooperation in Education and Research (OeAD-GmbH) Sparkling Science Grant [SPA-05/232]
  2. University of Veterinary Medicine Vienna
  3. Austrian Research Promotion Agency (FFG) [7269695]

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This study introduces an ovine model of tendon injury for comparing adult scarring repair and fetal regeneration. The results show that fetal tendons can completely regenerate within 28 days, while adult tendon defects remain evident five months post-injury. Proteome analyses reveal distinct differences in inflammation and repair processes between adult and fetal tendons, highlighting the potential therapeutic implications of understanding fetal healing mechanisms.
Tendinopathies are painful, disabling conditions that afflict 25% of the adult human population. Filling an unmet need for realistic large-animal models, we here present an ovine model of tendon injury for the comparative study of adult scarring repair and fetal regeneration. Complete regeneration of the fetal tendon within 28 days is demonstrated, while adult tendon defects remained macroscopically and histologically evident five months post-injury. In addition to a comprehensive histological assessment, proteome analyses of secretomes were performed. Confirming histological data, a specific and pronounced inflammation accompanied by activation of neutrophils in adult tendon defects was observed, corroborated by the significant up-regulation of pro-inflammatory factors, neutrophil attracting chemokines, the release of potentially tissue-damaging antimicrobial and extracellular matrix-degrading enzymes, and a response to oxidative stress. In contrast, secreted proteins of injured fetal tendons included proteins initiating the resolution of inflammation or promoting functional extracellular matrix production. These results demonstrate the power and relevance of our novel ovine fetal tendon regeneration model, which thus promises to accelerate research in the field. First insights from the model already support our molecular understanding of successful fetal tendon healing processes and may guide improved therapeutic strategies.

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