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从神经球培养的唐氏综合征(Ts1Cje)神经祖细胞中的增殖缺陷和基因表达失调

Proliferation deficits and gene expression dysregulation in Down's syndrome (Ts1Cje) neural progenitor cells cultured from neurospheres.

作者信息

Moldrich Randal X, Dauphinot Luce, Laffaire Julien, Vitalis Tania, Hérault Yann, Beart Philip M, Rossier Jean, Vivien Denis, Gehrig Corinne, Antonarakis Stylianos E, Lyle Robert, Potier Marie-Claude

机构信息

Laboratoire de Neurobiologie et Diversité Cellulaire, CNRS UMR7637, ESPCI, Paris, France.

出版信息

J Neurosci Res. 2009 Nov 1;87(14):3143-52. doi: 10.1002/jnr.22131.

Abstract

Down's syndrome neurophenotypes are characterized by mental retardation and a decreased brain volume. To identify whether deficits in proliferation could be responsible for this phenotype, neural progenitor cells were isolated from the developing E14 neocortex of Down's syndrome partial trisomy Ts1Cje mice and euploid (WT) littermates and grown as neurospheres. Ts1Cje neural progenitors proliferated at a slower rate, because of a longer cell cycle, and a greater number of cells were positive for glial fibrillary acidic protein. An increase in cell death was also noted. Gene expression profiles of neural progenitor cells from Ts1Cje and WT showed that 54% of triploid genes had expression ratios (Ts1Cje/WT) significantly greater than the expected diploid gene ratio of 1.0. Some diploid genes associated with proliferation, differentiation, and glial function were dysregulated. Interestingly, proliferation and gene expression dysregulation detected in the Ts1Cje mice did not require overexpression of the chromosome 21 genes amyloid precursor protein (App) and soluble superoxide dismutase 1 (Sod1).

摘要

唐氏综合征神经表型的特征是智力迟钝和脑容量减小。为了确定增殖缺陷是否可能导致这种表型,从唐氏综合征部分三体 Ts1Cje 小鼠和正常二倍体(野生型)同窝仔鼠发育中的 E14 新皮层中分离出神经祖细胞,并培养成神经球。由于细胞周期较长,Ts1Cje 神经祖细胞的增殖速度较慢,并且有更多细胞对胶质纤维酸性蛋白呈阳性。还注意到细胞死亡增加。Ts1Cje 和野生型神经祖细胞的基因表达谱显示,54% 的三倍体基因的表达比(Ts1Cje/野生型)显著高于预期的二倍体基因比 1.0。一些与增殖、分化和胶质细胞功能相关的二倍体基因表达失调。有趣的是,在 Ts1Cje 小鼠中检测到的增殖和基因表达失调并不需要 21 号染色体基因淀粉样前体蛋白(App)和可溶性超氧化物歧化酶 1(Sod1)的过表达。

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