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唐氏综合征中的转录紊乱:Ts1Cje小鼠小脑出生后发育的案例研究

Transcriptional disruptions in Down syndrome: a case study in the Ts1Cje mouse cerebellum during post-natal development.

作者信息

Potier M-C, Rivals I, Mercier G, Ettwiller L, Moldrich R X, Laffaire J, Personnaz L, Rossier J, Dauphinot L

机构信息

Unité Mixte de Recherche, 7637 Centre National de la Recherche Scientifique, Neurobiology, Paris, France.

出版信息

J Neurochem. 2006 Apr;97 Suppl 1:104-9. doi: 10.1111/j.1471-4159.2005.03624.x.

Abstract

To understand the aetiology and the phenotypic severity of Down syndrome, we searched for transcriptional signatures in a substructure of the brain (cerebellum) during post-natal development in a segmental trisomy 16 model, the Ts1Cje mouse. The goal of this study was to investigate the effects of trisomy on changes in gene expression across development time. The primary gene-dosage effect on triplicated genes (approximately 1.5) was observed at birth [post-natal day 0 (P0)], at P15 and P30. About 5% of the non-triplicated genes were significantly differentially expressed between trisomic and control cerebellum, while 25% of the transcriptome was modified during post-natal development of the cerebellum. Indeed, only 165, 171 and 115 genes were dysregulated in trisomic cerebellum at P0, P15 and P30, respectively. Surprisingly, there were only three genes dysregulated in development and in trisomic animals in a similar or opposite direction. These three genes (Dscr1, Son and Hmg14) were, quite unexpectedly, triplicated in the Ts1Cje model and should be candidate genes for understanding the aetiology of the phenotype observed in the cerebellum.

摘要

为了解唐氏综合征的病因及表型严重程度,我们在节段性16三体模型Ts1Cje小鼠出生后发育过程中,对大脑的一个亚结构(小脑)进行了转录特征研究。本研究的目的是调查三体性对整个发育时间内基因表达变化的影响。在出生时[出生后第0天(P0)]、P15和P30观察到对三倍体基因的主要基因剂量效应(约为1.5)。约5%的非三倍体基因在三体小脑和对照小脑中存在显著差异表达,而25%的转录组在小脑出生后发育过程中发生了改变。事实上,在P0、P15和P30时,三体小脑中分别只有165、171和115个基因表达失调。令人惊讶的是,在发育过程中和三体动物中,只有三个基因在相似或相反方向上表达失调。这三个基因(Dscr1、Son和Hmg14)在Ts1Cje模型中竟然是三倍体,应该是理解小脑中观察到的表型病因的候选基因。

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