4.6 Article

Soluble Collectin 11 (CL-11) Acts as an Immunosuppressive Molecule Potentially Used by Stem Cell-Derived Retinal Epithelial Cells to Modulate T Cell Response

Journal

CELLS
Volume 12, Issue 13, Pages -

Publisher

MDPI
DOI: 10.3390/cells12131805

Keywords

T cell activation; stem cell-derived retinal pigment epithelium cells; Collectin 11; transplantation

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Retinal pigment epithelium (RPE) cell allotransplantation is a potential solution for retinal diseases. However, the RPE-complement system triggered by CL-11 could hinder the success of transplantation due to the inflammatory response and T cell recognition promotion. We found that CL-11 inhibited T cell proliferation by binding to T cells and downregulating CD28 expression. Additionally, soluble CL-11 secreted by stressed RPE cells may contribute to the immunosuppressive properties of RPE cells.
Retinal pigment epithelium (RPE) cell allotransplantation is seen as a possible solution to retinal diseases. However, the RPE-complement system triggered by the binding of collectin-11 (CL-11) is a potential barrier for RPE transplantation as the complement-mediated inflammatory response may promote T cell recognition. To address this, we investigated the role of CL-11 on T cell immuno-response. We confirmed that RPE cells up-regulated MHC class I and expressed MHC class II molecules in an inflammatory setting. Co-cultures of RPE cells with T cells led to the inhibition of T cell proliferation. We found that CL-11 was partially responsible for this effect as T cell binding of CL-11 inhibited T cell proliferation in association with the downregulation of CD28. We also found that the suppressive action of CL-11 was abrogated in the presence of the RGD peptide given to block the T cell binding of CL-11 by its collagen-like domain. Because RPE cells can bind and secrete CL-11 under stress conditions, we postulate that soluble CL-11 contributes to the immunosuppressive properties of RPE cells. The investigation of this dual biological activity of CL-11, namely as a trigger of the complement cascade and a modulator of T cell responses, may provide additional clues about the mechanisms that orchestrate the immunogenic properties of RPE cells.

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