Abstract
Mesenchymal stromal cells (MSCs) are a promising therapeutic option for multiple immune diseases disorders; however, efficacy of MSC treatments can vary significantly. We present a novel licensing strategy to improve the immunosuppressive capacity of MSCs. Licensing murine MSCs with transforming growth factor-ß1 (TGF-ß MSCs) significantly improved their ability to modulate both the phenotype and secretome of inflammatory bone marrow-derived macrophages and significantly increased the numbers of regulatory T lymphocytes following co-culture assays. These TGF-ß MSC-expanded regulatory T lymphocytes also expressed significantly higher levels of PD-L1 and CD73, indicating enhanced suppressive potential. Detailed analysis of T lymphocyte co-cultures revealed modulation of secreted factors, most notably elevated prostaglandin E2 (PGE2). Furthermore, TGF-ß MSCs could significantly prolong rejection-free survival (69.2% acceptance rate compared to 21.4% for unlicensed MSC-treated recipients) in a murine corneal allograft model. Mechanistic studies revealed that (1) therapeutic efficacy of TGF-ß MSCs is Smad2 3-dependent, (2) the enhanced immunosuppressive capacity of TGF-ß MSCs is contact-dependent, and (3) enhanced secretion of PGE2 (via prostaglandin EP4 [E-type prostanoid 4] receptor) by TGF-ß MSCs is the predominant mediator of Treg expansion and T cell activation and is associated with corneal allograft survival. Collectively, we provide compelling evidence for the use of TGF-ß1 licensing as an unconventional strategy for enhancing MSC immunosuppressive capacity.
| Original language | English (Ireland) |
|---|---|
| Journal | Molecular Therapy : The Journal Of The American Society Of Gene Therapy |
| Volume | 28 |
| Issue number | 9 |
| DOIs | |
| Publication status | Published - 1 May 2020 |
Authors (Note for portal: view the doc link for the full list of authors)
- Authors
- Lynch K;Treacy O;Chen X;Murphy N;Lohan P;Islam MN;Donohoe E;Griffin MD;Watson L;McLoughlin S;O'Malley G;Ryan AE;Ritter T;
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