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2
Long-range formation of the Bicoid gradient requires multiple dynamic modes that spatially vary across the embryo.长程的 Bicoid 浓度梯度的形成需要多种动态模式,这些模式在胚胎中具有空间变化。
Development. 2024 Feb 1;151(3). doi: 10.1242/dev.202128. Epub 2024 Feb 12.
3
Intrinsic protein disorder is insufficient to drive subnuclear clustering in embryonic transcription factors.内在蛋白质无序不足以驱动胚胎转录因子的核内聚集。
Elife. 2024 Jan 26;12:RP88221. doi: 10.7554/eLife.88221.
4
Stepwise modifications of transcriptional hubs link pioneer factor activity to a burst of transcription.转录枢纽的逐步修饰将启动因子的活性与转录爆发联系起来。
Nat Commun. 2023 Aug 10;14(1):4848. doi: 10.1038/s41467-023-40485-6.
5
Dynamic phase separation of the androgen receptor and its coactivators key to regulate gene expression.雄激素受体及其共激活因子的动态相分离是调节基因表达的关键。
Nucleic Acids Res. 2023 Jan 11;51(1):99-116. doi: 10.1093/nar/gkac1158.
6
Thermodynamics predicts a stable microdroplet phase in polymer-gel mixtures undergoing elastic phase separation.热力学预测,在经历弹性相分离的聚合物-凝胶混合物中会出现一个稳定的微滴相。
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7
Transcription activation is enhanced by multivalent interactions independent of phase separation.转录激活通过多价相互作用增强,而与相分离无关。
Mol Cell. 2022 May 19;82(10):1878-1893.e10. doi: 10.1016/j.molcel.2022.04.017. Epub 2022 May 9.
8
Synthetic reconstruction of the promoter specifies the role of Bicoid, Zelda and Hunchback in the dynamics of its transcription.Synthetic 重建的 启动子指定了 Bicoid、Zelda 和 Hunchback 在其转录动力学中的作用。
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9
Following the tracks: How transcription factor binding dynamics control transcription.追踪转录因子结合动力学:如何控制转录。
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10
ERK signaling dissolves ERF repression condensates in living embryos.ERK 信号解除活胚胎中 ERF 抑制凝聚物。
Proc Natl Acad Sci U S A. 2022 Mar 1;119(9). doi: 10.1073/pnas.2119187119.

转录激活因子Bcd和阻遏因子Cic都会形成小型可移动的寡聚簇。

Both the transcriptional activator, Bcd, and repressor, Cic, form small mobile oligomeric clusters.

作者信息

Zhang Lili, Hodgins Lydia, Sakib Shariful, Verbeem Alexander, Mahmood Ahmad, Perez-Romero Carmina, Marmion Robert A, Dostatni Nathalie, Fradin Cécile

机构信息

Department of Physics and Astronomy, McMaster University, Hamilton, ON, Canada.

Department of Biochemistry and Biomedical Sciences, McMaster University, Hamilton, ON, Canada.

出版信息

Biophys J. 2025 Mar 18;124(6):980-995. doi: 10.1016/j.bpj.2024.08.011. Epub 2024 Aug 20.

DOI:10.1016/j.bpj.2024.08.011
PMID:39164967
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11947476/
Abstract

Transcription factors play an essential role in pattern formation during early embryo development, generating a strikingly fast and precise transcriptional response that results in sharp gene expression boundaries. To characterize the steps leading up to transcription, we performed a side-by-side comparison of the nuclear dynamics of two morphogens, a transcriptional activator, Bicoid (Bcd), and a transcriptional repressor, Capicua (Cic), both involved in body patterning along the anterior-posterior axis of the early Drosophila embryo. We used a combination of fluorescence recovery after photobleaching, fluorescence correlation spectroscopy, and single-particle tracking to access a wide range of dynamical timescales. Despite their opposite effects on gene transcription, we find that Bcd and Cic have very similar nuclear dynamics, characterized by the coexistence of a freely diffusing monomer population with a number of oligomeric clusters, which range from low stoichiometry and high mobility clusters to larger, DNA-bound hubs. Our observations are consistent with the inclusion of both Bcd and Cic into transcriptional hubs or condensates, while putting constraints on the mechanism by which these form. These results fit in with the recent proposal that many transcription factors might share a common search strategy for target gene regulatory regions that makes use of their large unstructured regions, and may eventually help explain how the transcriptional response they elicit can be at the same time so fast and so precise.

摘要

转录因子在早期胚胎发育过程中的模式形成中起着至关重要的作用,能产生极其快速且精确的转录反应,从而形成清晰的基因表达边界。为了描述转录之前的步骤,我们对两种形态发生素的核动力学进行了并行比较,这两种形态发生素分别是参与果蝇早期胚胎前后轴体模式形成的转录激活因子双胸蛋白(Bicoid,Bcd)和转录抑制因子卡皮库亚(Capicua,Cic)。我们结合使用了光漂白后的荧光恢复、荧光相关光谱和单粒子追踪技术,以获取广泛的动力学时间尺度。尽管它们对基因转录有相反的影响,但我们发现Bcd和Cic具有非常相似的核动力学,其特征是自由扩散的单体群体与许多寡聚簇共存,这些寡聚簇范围从低化学计量和高迁移率的簇到更大的与DNA结合的中心。我们的观察结果与将Bcd和Cic都纳入转录中心或凝聚物的观点一致,同时对它们形成的机制施加了限制。这些结果与最近的提议相符,即许多转录因子可能共享一种针对靶基因调控区域的共同搜索策略,该策略利用它们的大的无结构区域,并且最终可能有助于解释它们引发的转录反应如何能够同时如此快速和精确。