Inflammation activation and resolution in human tendon disease

Dakin, Stephanie G.; Martínez, Fernando O.; Yapp, Clarence; Wells, Graham; Oppermann, Udo; Dean, Benjamin; Smith, Robert S.; Wheway, Kim; Watkins, Bridget; Roche, S. Lucy; Carr, Andrew

doi:10.1126/scitranslmed.aac4269

Cited by 211 publications

(312 citation statements)

References 66 publications

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“…The matrix surrounding these cells is typically less well-structured, with inadequate hierarchical compartmentalization at the level of fascicles and above, and relatively disordered collagen structures at the level of fibers and below [192]. Additionally, the associated biochemical composition of the tissue may promote a chronic state of tissue inflammation, since among others pathological levels of collagen III with fewer cross links and increased presence of fragmented fibronectin are detected [191,[193][194][195][196][197][198][199]. At the levels of the tissue and organ, the effect of this aberrant tissue remodeling is an increased tendon crosssection that can provide adequate overall strength, but with suboptimal stiffness and function [8,[200][201][202][203].…”

Section: Tendon Damage and Repair: Intrinsic Microdamage Vs Damage Cmentioning

confidence: 99%

Tendon injury and repair – A perspective on the basic mechanisms of tendon disease and future clinical therapy

2017

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Section: Tendon Damage and Repair: Intrinsic Microdamage Vs Damage Cmentioning

confidence: 99%

Tendon injury and repair – A perspective on the basic mechanisms of tendon disease and future clinical therapy

2017

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“…8 However, there is growing support for the contribution of immune cells and inflammatory mediators to the development of tendinopathy. [9][10][11][12][13] Recent research showed that numbers of macrophages and mast cells are significantly increased in tendinopathic compared with healthy tendon tissues, and that inflammatory and fibrotic cytokines, peptides and growth factors have altered expression profiles in diseased compared with healthy tendons. 14 15 We recently reported that inflammatory signatures changed throughout different stages of severity in tissue samples from patients with supraspinatus tendinopathy.…”

Section: Introductionmentioning

confidence: 99%

Differential expression of alarmins—S100A9, IL-33, HMGB1 and HIF-1α in supraspinatus tendinopathy before and after treatment

Mosca

Carr

Snelling

et al. 2017

BMJ Open Sport Exerc Med

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BackgroundAlarmins, endogenous molecules released on tissue damage have been shown to play an important role in inflammatory musculoskeletal conditions including fracture repair andrheumatoid arthritis. However, the contribution of alarmins to the pathogenesis of tendon disease is not fully understood.MethodsWe investigated expression of alarmin proteins (S100A9, high-mobility group box 1 (HMGB1) and interleukin-33 (IL-33) and hypoxia-inducible factor 1α (HIF-1α), a subunit of an oxygen sensitive transcription factor, in three cohorts of human supraspinatus tissues: healthy (n=6), painful diseased (n=13) and post-treatment pain-free tendon samples (n=5). Tissue samples were collected during shoulder stabilisation surgery (healthy) or by biopsy needle (diseased/treated). Immunohistochemistry was used to investigate the protein expression of these factors in these healthy, diseased and treated tendons. Kruskal-Wallis with pairwise post hoc Mann-Whitney U tests were used to test for differences in immunopositive staining between these tissue cohorts. Additionally, costaining was performed to identify the cell types expressing HIF-1α, S100A9, IL-33 and HMGB1 in diseased tendons.ResultsImmunostaining showed HIF-1α and S100A9 were increased in diseased compared with healthy and post-treatment pain-free tendons (p<0.05). IL-33 was reduced in diseased compared with healthy tendons (p=0.0006). HMGB1 was increased in post-treatment pain-free compared with healthy and diseased tendons (p<0.01). Costaining of diseased tendon samples revealed that HIF-1α, S100A9 and IL-33 were expressed by CD68+ and CD68− cells, whereas HMGB1 was predominantly expressed by CD68− cells.ConclusionsThis study provides insight into the pathways contributing to the progressionand resolution of tendon disease. We found potential pro-inflammatory and pathogenic roles for HIF-1α and S100A9, a protective role fornuclear IL-33 and a potentially reparative function for HMGB1 in diseased supraspinatus tendons.

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“…Tendinopathy is one of the most common and most challenging problems for surgeons in orthopedics and sports medicine. Studies have reported that tendinopathy accounts for approximately 30% of sports injuries, and its pathogenesis is highly related to inflammation and degradation of connective tissue [14,15].…”

Section: Introductionmentioning

confidence: 99%

High Concentration of Aspirin Induces Apoptosis in Rat Tendon Stem Cells via Inhibition of the Wnt/β-Catenin Pathway

Wang

Tang

et al. 2018

Cell Physiol Biochem

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Background/Aims: Non-steroidal anti-inflammatory drugs (NSAIDs) are commonly used in clinical practice to relieve fever and pain. Aspirin, as a representative NSAID, has been widely used in the treatment of tendinopathy. Some reports have demonstrated that aspirin can induce apoptosis in cancer cells. However, evidence regarding aspirin treatment for tendinopathy, especially the effect of this treatment on tendon stem cells (TSCs), is lacking. Understanding the effect of aspirin on tendinopathy may provide a basis for the rational use of NSAIDs in clinical practice. The aim of our study was to determine whether aspirin induces apoptosis in rat TSCs via the Wnt/β-catenin pathway. Methods: First, we used flow cytometry and fluorescence to detect TSC apoptosis. Protein expression of the apoptosis-related caspase-3 pathway was investigated via western blot analysis. Next, we used western blotting to determine the effect of aspirin on the Wnt/β-catenin pathway. We used immunostaining to detect the levels of Bcl2, cleaved caspase-3, and P-β-catenin in the Achilles tendon. Finally, we used flow cytometry, fluorescence, and western blotting to investigate the aspirin-induced apoptosis of TSCs via the Wnt/β-catenin pathway. Results: Aspirin induced morphological apoptosis in rat TSCs via the mitochondrial/caspase-3 pathway and induced cellular apoptosis in the Achilles tendon. Apoptosis was partly reversed after adding the Wnt signaling activator Wnt3a and lithium chloride (LiCl, a GSK-3β inhibitor). Aspirin administration led to a dose-dependent increase in COX-2 expression. Apoptosis was promoted after adding the COX-2 inhibitor NS398. Conclusion: The Wnt/β-catenin pathway plays a vital role in aspirin-induced apoptosis by regulating mitochondrial/caspase-3 function. Elevating COX-2 levels may protect cells against apoptosis. More importantly, the results remind us to consider the apoptotic effect of aspirin on TSCs and tendon cells when aspirin is administered to treat tendinopathy. The relationship between the positive and negative effects of aspirin remains a subject for future study.

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Inflammation activation and resolution in human tendon disease

Cited by 211 publications

References 66 publications

Tendon injury and repair – A perspective on the basic mechanisms of tendon disease and future clinical therapy

Tendon injury and repair – A perspective on the basic mechanisms of tendon disease and future clinical therapy

Differential expression of alarmins—S100A9, IL-33, HMGB1 and HIF-1α in supraspinatus tendinopathy before and after treatment

High Concentration of Aspirin Induces Apoptosis in Rat Tendon Stem Cells via Inhibition of the Wnt/β-Catenin Pathway

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