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A cell surfaceome map for immunophenotyping and sorting pluripotent stem cells
Authors:Gundry Rebekah L  Riordon Daniel R  Tarasova Yelena  Chuppa Sandra  Bhattacharya Subarna  Juhasz Ondrej  Wiedemeier Olena  Milanovich Samuel  Noto Fallon K  Tchernyshyov Irina  Raginski Kimberly  Bausch-Fluck Damaris  Tae Hyun-Jin  Marshall Shannon  Duncan Stephen A  Wollscheid Bernd  Wersto Robert P  Rao Sridhar  Van Eyk Jennifer E  Boheler Kenneth R
Institution:Department of Biochemistry, Medical College of Wisconsin, Milwaukee, Wisconsin 53226, USA.
Abstract:Induction of a pluripotent state in somatic cells through nuclear reprogramming has ushered in a new era of regenerative medicine. Heterogeneity and varied differentiation potentials among induced pluripotent stem cell (iPSC) lines are, however, complicating factors that limit their usefulness for disease modeling, drug discovery, and patient therapies. Thus, there is an urgent need to develop nonmutagenic rapid throughput methods capable of distinguishing among putative iPSC lines of variable quality. To address this issue, we have applied a highly specific chemoproteomic targeting strategy for de novo discovery of cell surface N-glycoproteins to increase the knowledge-base of surface exposed proteins and accessible epitopes of pluripotent stem cells. We report the identification of 500 cell surface proteins on four embryonic stem cell and iPSCs lines and demonstrate the biological significance of this resource on mouse fibroblasts containing an oct4-GFP expression cassette that is active in reprogrammed cells. These results together with immunophenotyping, cell sorting, and functional analyses demonstrate that these newly identified surface marker panels are useful for isolating iPSCs from heterogeneous reprogrammed cultures and for isolating functionally distinct stem cell subpopulations.
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