کد مقاله | کد نشریه | سال انتشار | مقاله انگلیسی | نسخه تمام متن |
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6265421 | 1614081 | 2010 | 10 صفحه PDF | دانلود رایگان |

We hypothesized that one of the mechanisms underlying the protection of brain injury by therapeutic hypothermia is associated with preservation of neural stem cells. We investigated effects of moderate low temperature and the contribution of a cold-inducible molecule for the stemness of neural stem cells. The MEB5 mouse neural stem cell line was cultured in the presence or absence of EGF, and apoptosis, mRNA expression, and immunocytochemistry of the differentiation markers nestin and GFAP were evaluated at 37 or 32 °C. We investigated the contribution of the cold-inducible RNA binding protein (CIRP) on apoptosis and differentiation of MEB5 cells at 32 °C. EGF deprivation increased the number of apoptotic cells, decreased expression of nestin, and increased expression of GFAP. The moderate low temperature prevented apoptosis and decreases in expression of GFAP in MEB5 by EGF deprivation. The moderate low temperature significantly increased expression of CIRP. siRNA against CIRP significantly increased the apoptotic cell population of MEB5 cells via EGF deprivation at 32 °C. These findings suggest that moderate low temperature preserved stemness of neural stem cells and prevented cell apoptosis via the stimulation of CIRP, and one of the mechanisms of rescue of brain injury by the moderate hypothermia is associated with preservation of neural stem cells.
Research Highlights⺠The moderate low temperature prevented apoptosis and induced differentiation of neural stem cells in culture. ⺠The moderate low temperature increased expression of cold-inducible RNA binding protein (CIRP) in neural stem cells. ⺠Suppression of CIRP increased the apoptotic cell population of neural stem cells at moderate low temperature. ⺠One of the mechanisms of rescue of brain injury by the moderate hypothermia may be associated with preservation of neural stem cells.
Journal: Brain Research - Volume 1358, 28 October 2010, Pages 20-29