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Cited 36 time in webofscience Cited 42 time in scopus
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Comparison of Immunomodulation Properties of Porcine Mesenchymal Stromal/Stem Cells Derived from the Bone Marrow, Adipose Tissue, and Dermal Skin Tissueopen access

Authors
Ock, Sun-ASubbarao, Raghavendra BaregundiLee, Yeon-MiLee, Jeong-HyeonJeon, Ryoung-HoonLee, Sung-LimPark, Ji KwonHwang, Sun-ChulRho, Gyu-Jin
Issue Date
2016
Publisher
HINDAWI LTD
Citation
STEM CELLS INTERNATIONAL, v.2016
Indexed
SCIE
SCOPUS
Journal Title
STEM CELLS INTERNATIONAL
Volume
2016
URI
https://scholarworks.gnu.ac.kr/handle/sw.gnu/16804
DOI
10.1155/2016/9581350
ISSN
1687-966X
1687-9678
Abstract
Mesenchymal stromal/stem cells (MSCs) demonstrate immunomodulation capacity that has been implicated in the reduction of graft-versus-host disease. Accordingly, we herein investigated the capacity of MSCs derived from several tissue sources to modulate both proinflammatory (interferon [IFN] gamma and tumor necrosis factor [TNF] alpha) and immunosuppressive cytokines (transforming growth factor [TGF] beta and interleukin [IL] 10) employing xenogeneic human MSC-mixed lymphocyte reaction (MLR) test. Bone marrow-derived MSCs showed higher self-renewal capacity with relatively slow proliferation rate in contrast to adipose-derived MSCs which displayed higher proliferation rate. Except for the lipoprotein gene, there were no marked changes in osteogenesis-and adipogenesis-related genes following in vitro differentiation; however, the histological marker analysis revealed that adipose MSCs could be differentiated into both adipose and bone tissue. TGF beta and IL10 were detected in adipose MSCs and bone marrow MSCs, respectively. However, skin-derived MSCs expressed both IFN gamma and IL10, which may render them sensitive to immunomodulation. The xenogeneic human MLR test revealed that MSCs had a partial immunomodulation capacity, as proliferation of activated and resting peripheral blood mononuclear cells was not affected, but this did not differ among MSC sources. MSCs were not tumorigenic when introduced into immunodeficient mice. We concluded that the characteristics of MSCs are tissue source-dependent and their in vivo application requires more in-depth investigation regarding their precise immunomodulation capacities.
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