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在选择性染色质位点测定果蝇 Nrf2 和 GATA4 因子之间的复合物形成,证明转录共激活。

Determination of Complex Formation between Drosophila Nrf2 and GATA4 Factors at Selective Chromatin Loci Demonstrates Transcription Coactivation.

机构信息

Department of Biology, University of Minnesota Duluth, 1035 Kirby Drive, Duluth, MN 55812, USA.

出版信息

Cells. 2023 Mar 19;12(6):938. doi: 10.3390/cells12060938.

Abstract

Nrf2 is the dominant cellular stress response factor that protects cells through transcriptional responses to xenobiotic and oxidative stimuli. Nrf2 malfunction is highly correlated with many human diseases, but the underlying molecular mechanisms remain to be fully uncovered. GATA4 is a conserved GATA family transcription factor that is essential for cardiac and dorsal epidermal development. Here, we describe a novel interaction between Nrf2 and GATA4 proteins, i.e., cap'n'collar C (CncC) and Pannier (Pnr), respectively. Using the bimolecular fluorescence complementation (BiFC) assay-a unique imaging tool for probing protein complexes in living cells-we detected CncC-Pnr complexes in the nuclei of embryonic and salivary gland cells. Visualization of CncC-Pnr BiFC signals on the polytene chromosome revealed that CncC and Pnr tend to form complexes in euchromatic regions, with a preference for loci that are not highly occupied by CncC or Pnr alone. Most genes within these loci are activated by the CncC-Pnr BiFC, but not by individually expressed CncC or Pnr fusion proteins, indicating a novel mechanism whereby CncC and Pnr interact at specific genomic loci and coactivate genes at these loci. Finally, CncC-induced early lethality can be rescued by Pnr depletion, suggesting that CncC and Pnr function in the same genetic pathway during the early development of . Taken together, these results elucidate a novel crosstalk between the Nrf2 xenobiotic/oxidative response factor and GATA factors in the transcriptional regulation of development. This study also demonstrates that the polytene chromosome BiFC assay is a valuable tool for mapping genes that are targeted by specific transcription factor complexes.

摘要

Nrf2 是一种主要的细胞应激反应因子,可通过对外源物和氧化应激的转录反应来保护细胞。Nrf2 功能障碍与许多人类疾病高度相关,但潜在的分子机制仍有待充分揭示。GATA4 是一种保守的 GATA 家族转录因子,对于心脏和背侧表皮的发育是必不可少的。在这里,我们描述了 Nrf2 和 GATA4 蛋白之间的一种新的相互作用,即分别为 cap'n'collar C(CncC)和 Pannier(Pnr)。使用双分子荧光互补(BiFC)测定法——一种用于在活细胞中探测蛋白复合物的独特成像工具,我们在胚胎和唾液腺细胞的细胞核中检测到了 CncC-Pnr 复合物。在多线染色体上对 CncC-Pnr BiFC 信号的可视化显示,CncC 和 Pnr 倾向于在常染色质区域形成复合物,并且偏爱那些不由 CncC 或 Pnr 单独高度占据的位点。这些位点内的大多数基因都被 CncC-Pnr BiFC 激活,但不能被单独表达的 CncC 或 Pnr 融合蛋白激活,这表明了一种新的机制,即 CncC 和 Pnr 在特定的基因组位点相互作用,并在这些位点上共同激活基因。最后,CncC 诱导的早期致死性可以通过 Pnr 耗竭来挽救,这表明在 早期发育过程中,CncC 和 Pnr 发挥作用的遗传途径相同。总之,这些结果阐明了 Nrf2 外源性/氧化应激反应因子与 GATA 因子在发育转录调控中的一种新的串扰。本研究还表明,多线染色体 BiFC 测定法是一种用于绘制特定转录因子复合物靶向基因的有价值的工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bc72/10047698/940ac92c3cad/cells-12-00938-g001.jpg

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