| Literature DB >> 25376628 |
M Franquesa1, F K Mensah, R Huizinga, T Strini, L Boon, E Lombardo, O DelaRosa, J D Laman, J M Grinyó, W Weimar, M G H Betjes, C C Baan, M J Hoogduijn.
Abstract
Mesenchymal or stromal stem cells (MSC) interact with cells of the immune system in multiple ways. Modulation of the immune system by MSC is believed to be a therapeutic option for autoimmune disease and transplant rejection. In recent years, B cells have moved into the focus of the attention as targets for the treatment of immune disorders. Current B-cell targeting treatment is based on the indiscriminate depletion of B cells. The aim of this study was to examine whether human adipose tissue-derived MSC (ASC) interact with B cells to affect their proliferation, differentiation, and immune function. ASC supported the survival of quiescent B cells predominantly via contact-dependent mechanisms. Coculture of B cells with activated T helper cells led to proliferation and differentiation of B cells into CD19(+) CD27(high) CD38(high) antibody-producing plasmablasts. ASC inhibited the proliferation of B cells and this effect was dependent on the presence of T cells. In contrast, ASC directly targeted B-cell differentiation, independently of T cells. In the presence of ASC, plasmablast formation was reduced and IL-10-producing CD19(+) CD24(high) CD38(high) B cells, known as regulatory B cells, were induced. These results demonstrate that ASC affect B cell biology in vitro, suggesting that they can be a tool for the modulation of the B-cell response in immune disease.Entities:
Keywords: B cell; Immunomodulation; Mesenchymal stem cell; Plasmablast; Regulatory B cell (Breg)
Mesh:
Year: 2015 PMID: 25376628 DOI: 10.1002/stem.1881
Source DB: PubMed Journal: Stem Cells ISSN: 1066-5099 Impact factor: 6.277