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线粒体基因组在神经母细胞瘤细胞分化中的作用。

Participation of the mitochondrial genome in the differentiation of neuroblastoma cells.

作者信息

Vayssière J L, Cordeau-Lossouarn L, Larcher J C, Basseville M, Gros F, Croizat B

机构信息

Laboratoire de Biochimie Cellulaire, Collège de France, Paris.

出版信息

In Vitro Cell Dev Biol. 1992 Nov-Dec;28A(11-12):763-72. doi: 10.1007/BF02631065.

Abstract

Using clonal cell lines isolated from murine neuroblastoma C1300, we investigated the mitochondrial changes related to neuronal differentiation and, more generally, the role played by the mitochondrion in this phenomenon. By different approaches (measurement of the mitochondrial mass, immunoquantification of specific mitochondrial proteins, or incorporation of Rhodamine 123), the differentiation of the inducible clone, N1E-115, was found associated with an important increase of the cellular content in mitochondria. This increase could be observed with differentiating N1E-115 cells maintained in suspension, i.e. under conditions where neurite outgrowth is prevented but other early stages of (biochemical) differentiation continue to occur. That these mitochondrial changes are likely to be correlated with these stages of neuronal differentiation, rather than with simple progression to the postmitotic stage, stems from comparative experiments with clone N1A-103, a neuroblastoma cell line variant that becomes postmitotic after induction but fails to differentiate and shows no modification in its cellular content in mitochondria. In accordance with these observations, chloramphenicol prevents differentiation when added together with the inducer. This effect is probably related to the inhibition of mitochondrial translation rather than to modification of the bioenergetic needs because oligomycine, a potent inhibitor of the mitochondrial ATP synthetase, shows no effect on neurogenesis. As a working hypothesis and in keeping with independently published models, we postulate that products resulting from mitochondrial translation could be involved in the organization of the cytoskeleton or of certain membrane components whose rearrangements should be the prerequisite or the correlates to early stages of neuronal differentiation.

摘要

利用从小鼠神经母细胞瘤C1300分离出的克隆细胞系,我们研究了与神经元分化相关的线粒体变化,更广泛地说,研究了线粒体在这一现象中所起的作用。通过不同方法(线粒体质量测量、特定线粒体蛋白的免疫定量或罗丹明123掺入),发现可诱导克隆N1E-115的分化与细胞线粒体含量的显著增加有关。这种增加在悬浮培养的分化N1E-115细胞中也能观察到,即在防止神经突生长但(生化)分化的其他早期阶段仍继续发生的条件下。这些线粒体变化可能与神经元分化的这些阶段相关,而不是与简单进入有丝分裂后阶段相关,这源于与克隆N1A-103的对比实验,N1A-103是一种神经母细胞瘤细胞系变体,诱导后进入有丝分裂后阶段,但不能分化,其细胞线粒体含量也无变化。根据这些观察结果,氯霉素与诱导剂一起添加时可阻止分化。这种作用可能与线粒体翻译的抑制有关,而不是与生物能量需求的改变有关,因为线粒体ATP合成酶的强效抑制剂寡霉素对神经发生没有影响。作为一个工作假设并与独立发表的模型一致,我们推测线粒体翻译产生的产物可能参与细胞骨架或某些膜成分的组织,其重排应该是神经元分化早期阶段的前提条件或相关因素。

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