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测量位置信息的时间:母体驼背对于合子转录起始时 Bicoid 转录反应的同步性是必需的。

The time to measure positional information: maternal hunchback is required for the synchrony of the Bicoid transcriptional response at the onset of zygotic transcription.

机构信息

Institut Curie, Paris, F-75248 France.

出版信息

Development. 2010 Aug;137(16):2795-804. doi: 10.1242/dev.051300.

Abstract

It is widely accepted that morphogenetic gradients determine cell identity by concentration-dependent activation of target genes. How precise is each step in the gene expression process that acts downstream of morphogens, however, remains unclear. The Bicoid morphogen is a transcription factor directly activating its target genes and provides thus a simple system to address this issue in a quantitative manner. Recent studies indicate that the Bicoid gradient is precisely established in Drosophila embryos after eight nuclear divisions (cycle 9) and that target protein expression is specified five divisions later (cycle 14), with a precision that corresponds to a relative difference of Bicoid concentration of 10%. To understand how such precision was achieved, we directly analyzed nascent transcripts of the hunchback target gene at their site of synthesis. Most anterior nuclei in cycle 11 interphasic embryos exhibit efficient biallelic transcription of hunchback and this synchronous expression is specified within a 10% difference of Bicoid concentration. The fast diffusion of Bcd-EGFP (7.7 mum(2)/s) that we captured by fluorescent correlation spectroscopy in the nucleus is consistent with this robust expression at cycle 11. However, given the interruption of transcription during mitosis, it remains too slow to be consistent with precise de novo reading of Bicoid concentration at each interphase, suggesting the existence of a memorization process that recalls this information from earlier cycles. The two anterior maternal morphogens, Bicoid and Hunchback, contribute differently to this early response: whereas Bicoid provides dose-dependent positional information along the axis, maternal Hunchback is required for the synchrony of the response and is therefore likely to be involved in this memorization process.

摘要

人们普遍认为形态发生梯度通过靶基因的浓度依赖性激活来决定细胞身份。然而,形态发生素下游的基因表达过程的每一步有多精确尚不清楚。Bicoid 形态发生素是一种直接激活其靶基因的转录因子,因此为以定量方式解决这个问题提供了一个简单的系统。最近的研究表明,在八个核分裂(周期 9)后,Bicoid 形态发生素梯度在果蝇胚胎中被精确建立,并且靶蛋白表达在五个分裂后(周期 14)被指定,其精度对应于 Bicoid 浓度的相对差异为 10%。为了了解如何实现这种精度,我们直接在合成部位分析了 hunchback 靶基因的新生转录本。在周期 11 间期间胚胎的最前核中,hunchback 表现出有效的双等位基因转录,这种同步表达在 Bicoid 浓度的 10%差异内被指定。我们通过荧光相关光谱法在核内捕获到的 Bcd-EGFP(7.7 mum(2)/s)的快速扩散与周期 11 时的这种强大表达一致。然而,鉴于在有丝分裂过程中转录的中断,它仍然太慢,无法与每个间期间精确读取 Bicoid 浓度一致,这表明存在一种记忆过程,可从早期周期中回忆起该信息。两个前体母性形态发生素,Bicoid 和 Hunchback,对这种早期反应的贡献不同:虽然 Bicoid 沿着轴提供了剂量依赖性的位置信息,但母性 Hunchback 对于反应的同步性是必需的,因此可能参与了这种记忆过程。

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