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Title: Cord blood mesenchymal stem cells propel human dendritic cells to an intermediate maturation state and boost interleukin-12 production by mature dendritic cells.
Author(s): Berk, L.C.J. van den (289490820)
Roelofs, H.
Huijs, T. (314665625)
Siebers-Vermeulen, K.G.C. (314667288)
Raymakers, R.A.P. (298974371)
Kogler, G.
Figdor, C.G. (067631614)
Torensma, R. (068280769)
Publication year: 2009
Document type: Article / Letter to editor
Journal: Immunology
ISSN: 0019-2805
Volume: vol. 128
Issue: iss. 4
Start page: p. 564
End page: p. 572
Abstract: Pathogen-derived entities force the tissue-resident dendritic cells (DCs) towards a mature state, followed by migration to the draining lymph node to present antigens to T cells. Bone marrow mesenchymal stem cells (MSCs) modulate the differentiation, maturation and function of DCs. In umbilical cord blood an immature MSC population was identified. Remarkably, these immature stem cells modulated DCs in a different way. Marker expression was unchanged during the differentiation of monocytes towards immature DCs (iDCs) when cocultured with cord blood MSC [unrestricted somatic stem cells (USSCs)]. The maturation to mature DCs (mDCs) was enhanced when DCs were co-cultured with USSC, as evidenced by the up-regulation of costimulatory molecules. Endocytosis of dextran by iDCs was hampered in the presence of USSCs, which is indicative for the maturation of iDCs. Despite this maturation, the migration of iDCs cocultured with USSCs appeared to be identical to iDCs cultured alone. However, USSCs increased the migration of mDCs towards CCL21 and boosted interleukin-12 production. So, USSCs mature iDCs, thereby redirecting the antigen-uptake phenotype towards a mature phenotype. Furthermore, DC maturation by lipopolysaccharide (LPS) or USSCs reflects two distinct pathways because migration was unaffected when iDCs were matured by coculture with USSCs, while it was strongly enhanced in the presence of LPS. DCs are able to discriminate the different MSC subtypes, resulting in diverse differentiation programmes.
Subject: NCMLS 1B: Immune Regulation
NCMLS 1C: Tissue engineering and pathology
Organization: UMCN Extern
Haematology
Tumorimmunology
Appears in Collections:Academic bibliography

Please use this identifier to cite or link to this item: http://hdl.handle.net/2066/79681

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