Resumen
Dr. Robert K. Yu's research showed for the first time that the composition of glycosphingolipids is tightly regulated during embryo development. Studies in our group showed that the glycosphingolipid precursor ceramide is also critical for stem cell differentiation and apoptosis. Our new studies suggest that ceramide and its derivative, sphingosine-1-phosphate (S1P), act synergistically on embryonic stem (ES) cell differentiation. When using neural precursor cells (NPCs) derived from ES cells for transplantation, residual pluripotent stem (rPS) cells pose a significant risk of tumor formation after stem cell transplantation. We show here that rPS cells did not express the S1P receptor S1P1, which left them vulnerable to ceramide or ceramide analog (N-oleoyl serinol or S18)- induced apoptosis. In contrast, ES cell-derived NPCs expressed S1P1 and were protected in the presence of S1P or its pro-drug analog FTY720. Consistent with previous studies, FTY720-treated NPCs differentiated predominantly toward oligodendroglial lineage as tested by the expression of the oligodendrocyte precursor cell (OPC) markers Olig2 and O4. As the consequence, a combined administration of S18 and FTY720 to differentiating ES cells eliminated rPS cells and promoted oligodendroglial differentiation. In addition, we show that this combination promoted differentiation of ES cell-derived NPCs toward oligodendroglial lineage in vivo after transplantation into mouse brain.
| Idioma original | English |
|---|---|
| Páginas (desde-hasta) | 1601-1611 |
| Número de páginas | 11 |
| Publicación | Neurochemical Research |
| Volumen | 36 |
| N.º | 9 |
| DOI | |
| Estado | Published - sept 2011 |
Nota bibliográfica
Funding Information:Acknowledgments This work was supported in part by the NIH grants R01AG034389 and R01NS046835 to EB. The author also acknowledges institutional support (under directorship of Dr. Lin Mei) at the Medical College of Georgia/Georgia Health Sciences University, Augusta, GA. We are thankful to the Imaging Core Facility (under directorship of Dr. Paul McNeil) for assistance with confocal microscopy.
Financiación
Acknowledgments This work was supported in part by the NIH grants R01AG034389 and R01NS046835 to EB. The author also acknowledges institutional support (under directorship of Dr. Lin Mei) at the Medical College of Georgia/Georgia Health Sciences University, Augusta, GA. We are thankful to the Imaging Core Facility (under directorship of Dr. Paul McNeil) for assistance with confocal microscopy.
| Financiadores | Número del financiador |
|---|---|
| National Institutes of Health (NIH) | R01AG034389 |
| National Institute of Neurological Disorders and Stroke | R01NS046835 |
ASJC Scopus subject areas
- Biochemistry
- Cellular and Molecular Neuroscience
Huella
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