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金属反应转录因子 1(MTF-1)在镉抗性细胞中的基因组再分配。

Genomic Redistribution of Metal-Response Transcription Factor-1 (MTF-1) in Cadmium Resistant Cells.

机构信息

Department of Pharmacology, University of Colorado Anschutz Medical Campus, Aurora, CO 80045, USA.

出版信息

Cells. 2023 Mar 21;12(6):953. doi: 10.3390/cells12060953.

Abstract

(1) Background: Metal homeostasis is an important part of cellular programs and is disrupted when cells are exposed to carcinogenic heavy metals. Metal response is mediated by the metal response element transcription factor MTF-1. However, where MTF-1 binds and how that binding changes in response to heavy metals, such as cadmium, remains unknown. (2) Methods: To investigate the effects of prolonged cadmium exposure on the genomic distribution of MTF-1, we performed MTF-1 CUT&RUN, RNA-seq and ATAC-seq on control and cadmium-resistant cells. (3) Results: Changes in MTF-1 binding primarily occur distal to the transcription start sight. Newly occupied MTF-1 sites are enriched for FOS/JUN DNA binding motifs, while regions that lose MTF-1 binding in cadmium are enriched for the FOX transcription factor family member DNA binding sites. (4) Conclusions: Relocalization of MTF-1 to new genomic loci does not alter the accessibility of these locations. Our results support a model whereby MTF-1 is relocalized to accessible FOS/JUN-bound genomic locations in response to cadmium.

摘要

(1) 背景:金属内稳态是细胞程序的重要组成部分,当细胞暴露于致癌重金属时,金属内稳态会被破坏。金属反应是由金属反应元件转录因子 MTF-1 介导的。然而,MTF-1 结合的位置以及结合如何响应重金属(如镉)而改变尚不清楚。(2) 方法:为了研究长期镉暴露对 MTF-1 基因组分布的影响,我们对对照和镉抗性细胞进行了 MTF-1 CUT&RUN、RNA-seq 和 ATAC-seq 实验。(3) 结果:MTF-1 结合的变化主要发生在转录起始位点的远端。新占据的 MTF-1 位点富含 FOS/JUN DNA 结合基序,而在镉中失去 MTF-1 结合的区域富含 FOX 转录因子家族成员 DNA 结合位点。(4) 结论:MTF-1 向新的基因组位置的重定位不会改变这些位置的可及性。我们的结果支持这样一种模型,即在镉的作用下,MTF-1 被重新定位到可及的 FOS/JUN 结合的基因组位置。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d3c9/10047149/57df8ac4f735/cells-12-00953-g001.jpg

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