Targeting an Imbalance of Inflammatory Factors Induces Regeneration in Osteoarthritic Joints
Researchers here demonstrate that various cell populations found in osteoarthritic joint tissue remain competent and capable of regeneration, but these activities are suppressed by factors found in the local environment. Suspecting an excess of inflammatory signaling as the culprit, the researchers designed an anti-inflammatory cell therapy, employing cell types that act to counter inflammatory signaling. The results were promising in a mouse model of osteoarthritis, and continued to be promising in a small human clinical trial.
It can be hypothesized that functional regeneration of osteochondral defects may occur through the activation of appropriate progenitor cells recruited from the surrounding tissues, such as the synovial membrane, upon the onset of the pro-regenerative phase from the local immune cells. Once these progenitors are activated by trauma, they migrate to the defect site where they attach, proliferate, and undergo chondrogenic differentiation to contribute to tissue regeneration. Subsequently, it can be hypothesized that elements in the synovial environment of osteoarthritis (OA) may interfere with any of these crucial steps, impairing the regenerative potential. These elements would then be a cause, and as a result, a target to treat and potentially cure OA in a clinically effective way.
The synovial fluid (SF) from OA patients was herein identified to be a major inhibitor of the regenerative process in an OA environment. Specifically, the heterogeneous cell population isolated from the SF showed a clear ability to migrate, attach, proliferate, and undergo chondrogenic differentiation, all steps crucial for functional regeneration to occur, under standard assay conditions. However, the presence of autologous SF (aSF) during any of these events drastically impaired these processes. Characterization of the SF cytokine composition linked these results to a specific pro-inflammatory profile, suggesting an imbalance between pro- and anti-inflammatory immune cells in the SF.
On the basis of these findings, an immunomodulatory cell treatment was developed with the goal of restoring joint homeostasis by mimicking crucial events seen during tissue regeneration. The treatment was based on anti-inflammatory cartilage-activated T cells (CATs), which upon coculture with adipose-derived mesenchymal stromal cells (aMSCs), induced chondrogenic priming of the progenitor cells. Intra-articular injection of the final coculture steered articular cartilage regeneration and restored joint homeostasis in a rat OA model. A later clinical evaluation in human patients showed improved quality of life, reduced pain, and articular cartilage regeneration in a compassionate use study.
Can you provide a link to, or the name of the organization referred to in this article?
@Frank
Working link:
https://www.science.org/doi/10.1126/sciadv.ade4645
Acknowledgments
Funding: The research was funded partly by the Research Foundation - Flanders through research grant 1518618N, the postdoctoral grant 12S6817N, and the B.A.E.F. Henri Benedictus Fellowship.
Author contributions: J.B., G.M., and A.A. conceived and designed the study. J.B. and E.P. performed in vitro experiments and generated data. J.B., W.V., and G.M. performed in vivo experiments. J.B. and O.J. performed analysis from in vivo experiments. G.P. collected clinical SF samples and evaluated MRIs. M.T.M.B. managed clinical data. J.B. wrote the manuscript. O.J., W.V., G.M., E.P., and A.A. edited the manuscript. All authors read and approved the final draft of the manuscript.
Competing interests: The authors declare that they have no competing interests. A patent has been filed for the described cell therapy no. 63/279,316, Wake Forest University Health Sciences, with inventors: J.B., G.M., and A.A., 15 November 2021.
DOI not working? Michael
What is interesting about joint repair is to jumpstart the process you need a certain level of inflammation. Too little or too much or some other disbalance and you have degeneration instead of regeneration. On the other hand, there just so many possible pathways and eventually some researchers will find the last one...