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90 年的孕激素:孕激素受体在乳腺癌基因组上作用的分子机制。

90 YEARS OF PROGESTERONE: Molecular mechanisms of progesterone receptor action on the breast cancer genome.

机构信息

Centre de Regulació Genomica (CRG), Barcelona Institute of Science and Technology (BIST), Dr. Aiguader 88, Barcelona, Spain.

Universitat Pompeu Fabra (UPF), Barcelona, Spain.

出版信息

J Mol Endocrinol. 2020 Jul;65(1):T65-T79. doi: 10.1530/JME-19-0266.

Abstract

Gene regulation by steroid hormones has been at the forefront in elucidating the intricacies of transcriptional regulation in eukaryotes ever since the discovery by Karlson and Clever that the insect steroid hormone ecdysone induces chromatin puffs in giant chromosomes. After the successful cloning of the hormone receptors toward the end of the past century, detailed mechanistic insight emerged in some model systems, in particular the MMTV provirus. With the arrival of next generation DNA sequencing and the omics techniques, we have gained even further insight into the global cellular response to steroid hormones that in the past decades also extended to the function of the 3D genome topology. More recently, advances in high resolution microcopy, single cell genomics and the new vision of liquid-liquid phase transitions in the context of nuclear space bring us closer than ever to unravelling the logic of gene regulation and its complex integration of global cellular signaling networks. Using the function of progesterone and its cellular receptor in breast cancer cells, we will briefly summarize the history and describe the present extent of our knowledge on how regulatory proteins deal with the chromatin structure to gain access to DNA sequences and interpret the genomic instructions that enable cells to respond selectively to external signals by reshaping their gene regulatory networks.

摘要

类固醇激素的基因调控一直是阐明真核生物转录调控复杂性的前沿领域,自从 Karlson 和 Clever 发现昆虫类固醇激素蜕皮激素诱导巨大染色体中的染色质泡以来就是如此。在上个世纪末成功克隆激素受体之后,在一些模型系统中,特别是在 MMTV 前病毒中,出现了详细的机制见解。随着下一代 DNA 测序和组学技术的到来,我们对类固醇激素引起的细胞整体反应有了更深入的了解,在过去几十年中,这种反应也扩展到了 3D 基因组拓扑结构的功能。最近,高分辨率显微镜、单细胞基因组学以及核空间中液-液相转变的新观点,使我们比以往任何时候都更接近于揭示基因调控的逻辑及其与全球细胞信号网络的复杂整合。本文以孕激素及其在乳腺癌细胞中的细胞受体为例,简要总结了历史,并描述了我们目前对调节蛋白如何处理染色质结构以接触 DNA 序列以及解释基因组指令的认识程度,这些指令使细胞能够通过重塑其基因调控网络来选择性地对外界信号做出反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/624d/7354705/3d2b379fbd66/JME-19-0266fig1.jpg

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