生物
发起人
DNA去甲基化
增强子
CTCF公司
抄写(语言学)
分子生物学
原钙粘蛋白
转录因子
基因
DNA甲基化
遗传学
基因表达
细胞
哲学
钙粘蛋白
语言学
作者
Daniele Canzio,Chiamaka L. Nwakeze,Adan Horta,Sandy M. Rajkumar,Eliot L. Coffey,Erin E. Duffy,Rachel Duffié,Kevin D. Monahan,Sean O’Keeffe,Matthew D. Simon,Stavros Lomvardas,Tom Maniatis
出处
期刊:Cell
[Elsevier]
日期:2019-04-01
卷期号:177 (3): 639-653.e15
被引量:126
标识
DOI:10.1016/j.cell.2019.03.008
摘要
Stochastic activation of clustered Protocadherin (Pcdh) α, β, and γ genes generates a cell-surface identity code in individual neurons that functions in neural circuit assembly. Here, we show that Pcdhα gene choice involves the activation of an antisense promoter located in the first exon of each Pcdhα alternate gene. Transcription of an antisense long noncoding RNA (lncRNA) from this antisense promoter extends through the sense promoter, leading to DNA demethylation of the CTCF binding sites proximal to each promoter. Demethylation-dependent CTCF binding to both promoters facilitates cohesin-mediated DNA looping with a distal enhancer (HS5-1), locking in the transcriptional state of the chosen Pcdhα gene. Uncoupling DNA demethylation from antisense transcription by Tet3 overexpression in mouse olfactory neurons promotes CTCF binding to all Pcdhα promoters, resulting in proximity-biased DNA looping of the HS5-1 enhancer. Thus, antisense transcription-mediated promoter demethylation functions as a mechanism for distance-independent enhancer/promoter DNA looping to ensure stochastic Pcdhα promoter choice.
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