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异质性核因子-κB激活和增强子特征塑造免疫中的转录。

Heterogeneous NF-κB activation and enhancer features shape transcription in immunity.

作者信息

Nawar Noshin, Rits Emma, Cohen Lianne, Wunderlich Zeba

机构信息

Department of Biomedical Engineering, Boston University, Boston MA 02215, USA.

Biological Design Center, Boston University, Boston, MA 02215, USA.

出版信息

bioRxiv. 2025 May 19:2025.05.19.654881. doi: 10.1101/2025.05.19.654881.

Abstract

Conserved NF-κB signaling pathways shape immune responses in animals. In mammals, NF-κB activation patterns and downstream transcription vary with stimulus, cell type, and stochastic differences among identically treated cells. Whether animals without adaptive immunity exhibit similar heterogeneity or rely on distinct immune strategies remains unknown. We engineered S2* reporter cells as an immune-responsive model to monitor the dynamics of an NF-κB transcription factor, Relish, and downstream transcription in single, living cells. Following immune stimulation, Relish exhibits diverse nuclear localization dynamics that fall into distinct categories, with both the fraction of responsive cells and their activation speed rising with stimulus dose. Pre-stimulus features, including Relish nuclear fraction, predict a cell's responsiveness to stimulation. Simultaneous measurement of Relish and downstream transcription revealed that the probability of transcriptional bursts from immune-responsive enhancers correlates with Relish nuclear fraction. The number of NF-κB binding sites tunes transcriptional activity among immune enhancers. Our study uncovers heterogeneity in NF-κB activation and target gene expression within , illustrating how dynamic NF-κB behavior and enhancer architecture tune gene regulation.

摘要

保守的NF-κB信号通路塑造动物的免疫反应。在哺乳动物中,NF-κB的激活模式和下游转录因刺激、细胞类型以及相同处理细胞间的随机差异而有所不同。缺乏适应性免疫的动物是否表现出类似的异质性或依赖于不同的免疫策略仍不清楚。我们构建了S2*报告细胞作为免疫反应模型,以监测单个活细胞中NF-κB转录因子Relish的动态变化及其下游转录。免疫刺激后,Relish表现出多样的核定位动态,可分为不同类别,响应细胞的比例及其激活速度均随刺激剂量增加而升高。刺激前的特征,包括Relish核比例,可预测细胞对刺激的反应性。对Relish和下游转录的同时测量表明,免疫反应增强子转录爆发的概率与Relish核比例相关。NF-κB结合位点的数量调节免疫增强子之间的转录活性。我们的研究揭示了NF-κB激活和靶基因表达在[此处原文缺失相关内容]内的异质性,阐明了动态的NF-κB行为和增强子结构如何调节基因表达。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/561b/12139968/8c581c285c55/nihpp-2025.05.19.654881v1-f0001.jpg

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