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Immunomodulatory Contribution of Mast Cells to the Regenerative Biomaterial Microenvironment
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AbstractBioactive immunomodulatory biomaterials have shown promise for influencing the immune response to promote tissue repair and regeneration. Macrophages and T cells have been associated with this response; however, other immune cell types have been traditionally overlooked. In this study, we investigated the role of mast cells in the regulation of the immune response to decellularized biomaterial scaffolds using a subcutaneous implant model. In mast cell-deficient mice, there was dysregulation of the expected M1 to M2 macrophage transition typically induced by the biomaterial scaffold. Polarization progression deviated in a sex specific manner with an early transition to an M2 profile in female mice, while the male response was unable to properly transition past a pro-inflammatory M1 state. Both were reversed with adoptive mast cell transfer. Further investigation of the later stage immune response in male mice determined a greater sustained pro-inflammatory gene expression profile including the IL-1 cytokine family, IL-6, alarmins, and chemokines. These results highlight mast cells as another important cell type that influences the immune response to pro-regenerative biomaterials.
Cold Spring Harbor Laboratory
Title: Immunomodulatory Contribution of Mast Cells to the Regenerative Biomaterial Microenvironment
Description:
AbstractBioactive immunomodulatory biomaterials have shown promise for influencing the immune response to promote tissue repair and regeneration.
Macrophages and T cells have been associated with this response; however, other immune cell types have been traditionally overlooked.
In this study, we investigated the role of mast cells in the regulation of the immune response to decellularized biomaterial scaffolds using a subcutaneous implant model.
In mast cell-deficient mice, there was dysregulation of the expected M1 to M2 macrophage transition typically induced by the biomaterial scaffold.
Polarization progression deviated in a sex specific manner with an early transition to an M2 profile in female mice, while the male response was unable to properly transition past a pro-inflammatory M1 state.
Both were reversed with adoptive mast cell transfer.
Further investigation of the later stage immune response in male mice determined a greater sustained pro-inflammatory gene expression profile including the IL-1 cytokine family, IL-6, alarmins, and chemokines.
These results highlight mast cells as another important cell type that influences the immune response to pro-regenerative biomaterials.
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