Assessing the immunosuppressive activity of alginate-encapsulated mesenchymal stromal cells on splenocytes

被引:1
|
作者
Moise, Sandhya [1 ,2 ]
Dolcetti, Luigi [3 ]
Dazzi, Francesco [4 ]
Roach, Paul [5 ]
Buttery, Lee [6 ]
MacNeil, Sheila [7 ]
Medcalf, Nick [8 ]
机构
[1] Univ Bath, Ctr Integrated Bioproc Res CIBR, Dept Chem Engn, Bath, Avon, England
[2] Univ Bath, Ctr Therapeut Innovat CTI, Bath, Avon, England
[3] Kings Coll London, Dept Med & Pharmaceut Sci, London, England
[4] Kings Coll Hosp NHS Trust, Dept Haematol Malignancies & Stem Cell Transplant, London, England
[5] Loughborough Univ, Dept Chem, Loughborough, Leics, England
[6] Univ Nottingham, Sch Pharm, Nottingham, England
[7] Univ Sheffield, Kroto Res Inst, Dept Mat Sci & Engn, Biomat & Tissue Engn Grp, Sheffield, S Yorkshire, England
[8] Wolfson Sch Mech Elect & Mfg Engn, Ctr Biol Engn, Loughborough, Leics, England
关键词
Mesenchymal stromal cells; immunosuppression; alginate; splenocytes; encapsulation; STEM-CELLS; CHEMOKINES;
D O I
10.1080/21691401.2022.2088547
中图分类号
Q81 [生物工程学(生物技术)]; Q93 [微生物学];
学科分类号
071005 ; 0836 ; 090102 ; 100705 ;
摘要
Mesenchymal stromal cells (MSCs) show immunosuppressive effects both via cell-to-cell contact (direct) with immune cells and by producing paracrine factors and extracellular vesicles (indirect). A key challenge in delivering this therapeutic effect in vivo is retaining the MSCs at the site of injection. One way to address this is by encapsulating the MSCs within suitable biomaterial scaffolds. Here, we assess the immunosuppressive effect of alginate-encapsulated murine MSCs on proliferating murine splenocytes. Our results show that MSCs are able to significantly suppress splenocyte proliferation by similar to 50% via the indirect mechanism and almost completely (similar to 98%) via the direct mechanism. We also show for the first time that MSCs as monolayers on tissue culture plastic or encapsulated within alginate, when physically isolated from the splenocytes via transwells, are able to sustain immunosuppressive activity with repeated exposure to fresh splenocytes, for as long as 9 days. These results indicate the need to identify design strategies to simultaneously deliver both modes of MSC immunosuppression. By designing cell-biomaterial constructs with tailored degradation profiles, we can achieve a more sustained (avoiding MSCs migration and apoptosis) and controlled release of both the paracrine signals and eventually the cells themselves enabling efficient MSC-based immunosuppressive therapies for wound healing.
引用
收藏
页码:168 / 176
页数:9
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