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Stem cells act through multiple mechanisms to benefit mice with neurodegenerative metabolic disease
Authors:Lee Jean-Pyo  Jeyakumar Mylvaganam  Gonzalez Rodolfo  Takahashi Hiroto  Lee Pei-Jen  Baek Rena C  Clark Dan  Rose Heather  Fu Gerald  Clarke Jonathan  McKercher Scott  Meerloo Jennifer  Muller Franz-Josef  Park Kook In  Butters Terry D  Dwek Raymond A  Schwartz Philip  Tong Gang  Wenger David  Lipton Stuart A  Seyfried Thomas N  Platt Frances M  Snyder Evan Y
Affiliation:Stem Cell & Regeneration Program, Center for Neuroscience and Aging Research, Burnham Institute for Medical Research, La Jolla, California 92037, USA.
Abstract:Intracranial transplantation of neural stem cells (NSCs) delayed disease onset, preserved motor function, reduced pathology and prolonged survival in a mouse model of Sandhoff disease, a lethal gangliosidosis. Although donor-derived neurons were electrophysiologically active within chimeric regions, the small degree of neuronal replacement alone could not account for the improvement. NSCs also increased brain beta-hexosaminidase levels, reduced ganglioside storage and diminished activated microgliosis. Additionally, when oral glycosphingolipid biosynthesis inhibitors (beta-hexosaminidase substrate inhibitors) were combined with NSC transplantation, substantial synergy resulted. Efficacy extended to human NSCs, both to those isolated directly from the central nervous system (CNS) and to those derived secondarily from embryonic stem cells. Appreciating that NSCs exhibit a broad repertoire of potentially therapeutic actions, of which neuronal replacement is but one, may help in formulating rational multimodal strategies for the treatment of neurodegenerative diseases.
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