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温度通过 A20 转录的时间来调节 NF-κB 的动态和功能。

Temperature regulates NF-κB dynamics and function through timing of A20 transcription.

机构信息

Systems Microscopy Centre, Division of Molecular and Cellular Function, School of Biology, Faculty of Biology, Medicine and Health, Manchester Academic Health Sciences Centre, University of Manchester, M13 9PT Manchester, United Kingdom.

Mathematics Institute, University of Warwick, CV4 7AL Coventry, United Kingdom.

出版信息

Proc Natl Acad Sci U S A. 2018 May 29;115(22):E5243-E5249. doi: 10.1073/pnas.1803609115. Epub 2018 May 14.

Abstract

NF-κB signaling plays a pivotal role in control of the inflammatory response. We investigated how the dynamics and function of NF-κB were affected by temperature within the mammalian physiological range (34 °C to 40 °C). An increase in temperature led to an increase in NF-κB nuclear/cytoplasmic oscillation frequency following Tumor Necrosis Factor alpha (TNFα) stimulation. Mathematical modeling suggested that this temperature sensitivity might be due to an A20-dependent mechanism, and A20 silencing removed the sensitivity to increased temperature. The timing of the early response of a key set of NF-κB target genes showed strong temperature dependence. The cytokine-induced expression of many (but not all) later genes was insensitive to temperature change (suggesting that they might be functionally temperature-compensated). Moreover, a set of temperature- and TNFα-regulated genes were implicated in NF-κB cross-talk with key cell-fate-controlling pathways. In conclusion, NF-κB dynamics and target gene expression are modulated by temperature and can accurately transmit multidimensional information to control inflammation.

摘要

NF-κB 信号通路在炎症反应的控制中起着关键作用。我们研究了哺乳动物生理范围内(34°C 至 40°C)温度如何影响 NF-κB 的动力学和功能。TNFα 刺激后,温度升高导致 NF-κB 核/质振荡频率增加。数学模型表明,这种温度敏感性可能是由于 A20 依赖性机制,而 A20 沉默消除了对温度升高的敏感性。一组关键的 NF-κB 靶基因的早期反应的时间具有很强的温度依赖性。细胞因子诱导的许多(但不是全部)晚期基因的表达对温度变化不敏感(表明它们可能在功能上具有温度补偿)。此外,一组受温度和 TNFα 调控的基因与 NF-κB 与关键细胞命运控制途径的交叉对话有关。总之,NF-κB 的动力学和靶基因表达受温度调节,并能准确传递多维信息以控制炎症。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7e19/5984538/8b6721018a04/pnas.1803609115fig01.jpg

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