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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Progenitor cell injury after irradiation to the developing brain can be modulated by mild hypothermia or hyperthermia.
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Progenitor cell injury after irradiation to the developing brain can be modulated by mild hypothermia or hyperthermia.

机译:照射到发育中的大脑后,祖细胞损伤可通过轻度低温或高温来调节。

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Ionizing radiation induced acute cell death in the dentate gyrus subgranular zone (SGZ) and the subventricular zone (SVZ). Hypomyelination was also observed. The effects of mild hypothermia and hyperthermia for 4 h after irradiation (IR) were studied in postnatal day 9 rats. One hemisphere was irradiated with a single dose of 8 Gy and animals were randomized to normothermia (rectal temperature 36 degrees C for 4 h), hypothermia (32 degrees C for 4 h) or hyperthermia (39 degrees C for 4 h). Cellular injury, e.g. chromatin condensation and nitrotyrosine formation, appeared to proceed faster when the body temperature was higher. Caspase-3 activation was more pronounced in the hyperthermia group and nuclear translocation of p53 was less pronounced in the hypothermia group 6 h after IR. In the SVZ the loss of nestin-positive progenitors was more pronounced (48%) and the size was smaller (45%) in the hyperthermia group 7 days post-IR. Myelination was not different after hypo- or hyperthermia. This is the first report to demonstrate that hypothermia may be beneficial and that hyperthermia may aggravate the adverse side-effects after radiation therapy to the developing brain.
机译:电离辐射诱导齿状回亚颗粒区(SGZ)和脑室下区(SVZ)的急性细胞死亡。还观察到髓鞘过少。在出生后第9天的大鼠中研究了辐射(IR)后4 h的亚低温和高热的影响。用单剂量的8 Gy照射一个半球,并将动物随机分为正常体温(直肠温度36摄氏度,持续4小时),体温过低(32摄氏度,持续4小时)或体温过高(39摄氏度,持续4小时)。细胞损伤,例如当体温较高时,染色质凝结和硝基酪氨酸的形成似乎进行得更快。 IR后6小时,高热组中Caspase-3的激活更为明显,而低热组中p53的核转位则较不明显。在SVZ中,IR术后7天,热疗组中Nestin阳性祖细胞的丢失更为明显(48%),而大小更小(45%)。体温过低或过高后,髓鞘形成没有区别。这是第一份证明体温过低可能有益并且体温过高可能加重对发展中的脑部放射治疗后的不良副作用的报道。

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