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The correlation between human adipose-derived stem cells differentiation and cell adhesion mechanism
Authors:In-Su Park   Min Han   Jong-Won Rhie   Soo Hyun Kim   Youngmee Jung   Ik Hwan Kim  Sang-Heon Kim  
Affiliation:aBiomaterial Research Center, Division of Life Sciences, Korea Institute of Science and Technology, 39-1 Hawolgok, Seongbuk, Seoul 136-791, Republic of Korea;bDepartment of Plastic Surgery, College of Medicine, The Catholic University of Korea, Seoul 137-701, Republic of Korea;cSchool of Life Science and Biotechnology, Korea University, Seoul 136-701, Republic of Korea
Abstract:In recent years, research in the areas of stem cells has dramatically increased, including studies of cellular adhesion to a substrate. We sought to determine the adhesive properties of human adipose-derived stem cells (hASCs) for extracellular matrix proteins. The adhesion of hASCs to collagens and laminin was completely inhibited by a monoclonal antibody, Mab 2253, which binds to the β1 integrin subunit. These data indicate that hASC adhesion to collagens and laminin was exclusively mediated by an integrin. Cell adhesion on fibronectin (Fn) was inhibited by the heparin-binding peptide (HBP) in the presence of Mab 2253, but not by either Mab 2253 or HBP alone. These results indicate that both the β1 subunit and the heparan sulfate proteoglycan participated in the cell adhesion to Fn. Microscopic views showed extensive spreading of hASCs cultured on Fn, whereas the cells maintained a round shape when cultured on a heparin-binding domain (HBD) substrate. hASCs differentiated into adipocytes, which stained positive for lipid vacuoles by Oil Red-O analysis, more readily on HBD substrate than on FN substrate. These results suggest that hASCs have an adhesion mechanism for the HBD of Fn and hASC morphology is controlled by the adhesion mechanism and strongly correlated with adipogenic differentiation.
Keywords:Cell adhesion substrate   Human adipose-derived stem cells   Extracellular matrix   Fibronectin   Heparin-binding domain   Cell differentiation
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