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细胞因子对海马祖细胞神经元分化的调控

Cytokine regulation of neuronal differentiation of hippocampal progenitor cells.

作者信息

Mehler M F, Rozental R, Dougherty M, Spray D C, Kessler J A

机构信息

Department of Neurology, Albert Einstein College of Medicine, Bronx, New York 10461.

出版信息

Nature. 1993 Mar 4;362(6415):62-5. doi: 10.1038/362062a0.

Abstract

The signalling mechanisms governing haematolymphopoiesis and those regulating neural development may be closely related, as indicated by similarities of higher-order structure and function of the cytokines involved, of the regional and temporal regulation of their transcription and translation, and of their bioactivity. Here we investigate this possible evolutionary connection using retroviral transduction of a temperature-sensitive mutant form of the SV40 large T antigen to develop conditionally immortalized murine embryonic hippocampal progenitor cell lines. Treatment of these cells with cytokines that are thought to participate in progressive lymphoid maturation, immunoglobulin synthesis and erythropoiesis causes progressive neuronal differentiation, as defined by morphological criteria, successive expression of increasingly mature neurofilament protein, and the generation of inward currents and action potentials. The cytokine interleukin(IL)-11 induces expression of action potentials that are insensitive to tetrodotoxin, which is indicative of developmentally immature sodium channels. By contrast, for expression of more mature action potentials (tetrodotoxin-sensitive) one of the interleukins IL-5, IL-7 or IL-9 must be applied in association with transforming growth factor-alpha after pretreatment with basic fibroblast growth factor. Our results suggest that the mechanisms regulating lineage commitment and cellular differentiation in the neural and haematopoietic systems are similar. Further, they define an in vitro model system that may facilitate molecular analysis of graded stages of mammalian neuronal differentiation.

摘要

控制造血淋巴生成的信号机制与调节神经发育的信号机制可能密切相关,这一点可从相关细胞因子在高阶结构和功能、转录和翻译的区域及时间调控以及生物活性方面的相似性得到证明。在此,我们利用温度敏感型突变形式的SV40大T抗原进行逆转录病毒转导,以建立条件永生化的小鼠胚胎海马祖细胞系,从而研究这种可能的进化联系。用被认为参与渐进性淋巴细胞成熟、免疫球蛋白合成和红细胞生成的细胞因子处理这些细胞,会导致渐进性神经元分化,其定义依据形态学标准、逐渐成熟的神经丝蛋白的连续表达以及内向电流和动作电位的产生。细胞因子白细胞介素(IL)-11诱导产生对河豚毒素不敏感的动作电位,这表明存在发育不成熟的钠通道。相比之下,为了表达更成熟的动作电位(对河豚毒素敏感),在先用碱性成纤维细胞生长因子预处理后,必须联合应用白细胞介素IL-5、IL-7或IL-9之一与转化生长因子-α。我们的结果表明,调节神经和造血系统中谱系定向和细胞分化的机制是相似的。此外,它们定义了一个体外模型系统,该系统可能有助于对哺乳动物神经元分化的分级阶段进行分子分析。

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