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牛磺酸可刺激培养的小鼠胚胎神经祖细胞的增殖。

Taurine stimulates proliferation of mice embryonic cultured neural progenitor cells.

机构信息

División de Neurociencias, Instituto de Fisiología Celular, Universidad Nacional Autónoma de México, México City, México.

出版信息

J Neurosci Res. 2010 Jun;88(8):1673-81. doi: 10.1002/jnr.22328.

Abstract

Taurine is present in high levels in fetal brain which decrease in the adult, suggesting its role in brain development. In some regions of taurine deficient animals cells show defective migration and the presence of numerous mitotic figures, suggesting a delay in cell proliferation. To know more about the role of taurine in the developing brain cells, the present study investigated whether taurine is a factor involved in proliferation or/and viability of neural progenitor cells (NPC). NPC were obtained from 13.5-days mice embryos mesencephalon, and cultured during 4-5 days to form neurospheres in the presence of EGF plus FGFb (EGF/FGF) or EGF alone. Mesencephalon taurine content (349 mmoles/kg protein) was lost in NPC and recovered after addition of 10 mM taurine to the culture. Neurospheres-forming NPC were over 94% nestin-positive. Taurine increased 38.6% and 43.2% the number of NPC formed in EGF/FGF or EGF conditions, respectively. In secondary neurospheres this increase was 24.6% and 62.1%, in EGF/FGF or EGF cultures respectively. Correspondingly neurospheres size was increased by taurine but neurospheres number was not enhanced. Taurine significantly increased the number of BrdU-positive cells, without affecting cell viability, suggesting proliferation as the mechanism responsible for taurine action increasing NPC. Taurine seems unable to increase the number of beta-III-tubulin-positive cells differentiated from neurospheres after serum addition, and rather an increase in astrocytes was observed. These results point to taurine as a trophic factor contributing to optimize NPC proliferation.

摘要

牛磺酸在胎脑中的含量很高,在成年后会降低,这表明它在大脑发育中发挥作用。在某些牛磺酸缺乏动物的区域,细胞显示出迁移缺陷和大量有丝分裂图,表明细胞增殖延迟。为了更多地了解牛磺酸在发育中脑细胞中的作用,本研究调查了牛磺酸是否是参与神经祖细胞(NPC)增殖或/和存活的因素。NPC 从 13.5 天的胎鼠中获得,从中脑培养 4-5 天,在 EGF 和 FGFb(EGF/FGF)或 EGF 单独存在的情况下形成神经球。中脑中的牛磺酸含量(349mmol/kg 蛋白)在 NPC 中丢失,加入 10mM 牛磺酸后可恢复。神经球形成 NPC 的巢蛋白阳性率超过 94%。牛磺酸分别增加了 EGF/FGF 或 EGF 条件下形成的 NPC 数量增加了 38.6%和 43.2%。在次级神经球中,EGF/FGF 或 EGF 培养物中分别增加了 24.6%和 62.1%。相应地,牛磺酸增加了神经球的大小,但不增加神经球的数量。牛磺酸显著增加了 BrdU 阳性细胞的数量,而不影响细胞活力,表明增殖是牛磺酸增加 NPC 的作用机制。牛磺酸似乎无法增加血清添加后从神经球分化的β-III-微管蛋白阳性细胞的数量,而是观察到星形胶质细胞的增加。这些结果表明牛磺酸是一种营养因子,有助于优化 NPC 的增殖。

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