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Please use this identifier to cite or link to this item:
http://hdl.handle.net/10171/18353
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| Title: | Thymidine Analogs Are Transferred from Prelabeled Donor to Host Cells in the Central Nervous System After Transplantation: A Word of Caution |
| Author(s) : | Bruns, T. (T.C.) Ortiz-Gonzalez, X.R. (Xilma R.) Gutierrez-Perez, M. (María) Keene, C. (C.D.) Sharda, R. (Rohit) Demorest, Z. (Z.L.) Jiang, Y. (Y.) Nelson-Holte, M. (Molly) Soriano, M. (Mario) Nakagawa, Y. (Yasushi) Luquin, M.R. (María Rosario) García-Verdugo, J.M. (José Manuel) Prosper, F. (Felipe) Low, W.C. (Walter C.) Verfaillie, C.M. (Catherine M.) |
| Issue Date: | 2006 |
| Publisher: | Wiley-Blackwell |
| Citation: | Burns, T. C., Ortiz-Gonzalez, X. R., Gutierrez-Perez, M., Keene, C. D. et al. Thymidine Analogs Are Transferred from Prelabeled Donor to Host Cells in the Central Nervous System After Transplantation: A Word of Caution. Stem Cells 2006; 24 (4): 1121–1127 |
| Keywords: | Adult bone marrow stem cells Label Bromodeoxyuridine Thymidine analog Control Transplantation Neural differentiation In vivo tracking |
| Abstract: | Thymidine analogs, including bromodeoxyuridine, chlorodeoxyuridine,
iododeoxyuridine, and tritiated thymidine, label
dividing cells by incorporating into DNA during S phase of cell
division and are widely employed to identify cells transplanted
into the central nervous system. However, the potential for
transfer of thymidine analogs from grafted cells to dividing
host cells has not been thoroughly tested. We here demonstrate
that graft-derived thymidine analogs can become incorporated
into host neural precursors and glia. Large numbers of labeled
neurons and glia were found 3–12 weeks after transplantation
of thymidine analog-labeled live stem cells, suggesting differentiation
of grafted cells. Remarkably, however, similar results
were obtained after transplantation of dead cells or labeled
fibroblasts. Our findings reveal for the first time that thymidine
analog labeling may not be a reliable means of identifying
transplanted cells, particularly in highly proliferative environments
such as the developing, neurogenic, or injured brain. |
| URI: | http://hdl.handle.net/10171/18353 |
| Publisher version (URL): | http://dx.doi.org/10.1634/stemcells.2005-0463 |
| Appears in Collections: | DA - CIMA - Oncología - Síndromes mieloproliferativos - Artículos de Revista DA - CIMA - Oncología - Terapia celular - Artículos de Revista DA - CUN - Área de Terapia Celular - Artículos de revista DA - Medicina - Hematología - Artículos de revista
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