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糖皮质激素受体调控的增强子在药物成瘾相关基因调控网络中起核心作用。

Glucocorticoid Receptor-Regulated Enhancers Play a Central Role in the Gene Regulatory Networks Underlying Drug Addiction.

作者信息

Duttke Sascha H, Montilla-Perez Patricia, Chang Max W, Li Hairi, Chen Hao, Carrette Lieselot L G, de Guglielmo Giordano, George Olivier, Palmer Abraham A, Benner Christopher, Telese Francesca

机构信息

Department of Medicine, University of California, San Diego, La Jolla, CA, United States.

School of Molecular Biosciences, College of Veterinary Medicine, Washington State University, Pullman, WA, United States.

出版信息

Front Neurosci. 2022 May 16;16:858427. doi: 10.3389/fnins.2022.858427. eCollection 2022.

Abstract

Substance abuse and addiction represent a significant public health problem that impacts multiple dimensions of society, including healthcare, the economy, and the workforce. In 2021, over 100,000 drug overdose deaths were reported in the US, with an alarming increase in fatalities related to opioids and psychostimulants. Understanding the fundamental gene regulatory mechanisms underlying addiction and related behaviors could facilitate more effective treatments. To explore how repeated drug exposure alters gene regulatory networks in the brain, we combined capped small (cs)RNA-seq, which accurately captures nascent-like initiating transcripts from total RNA, with Hi-C and single nuclei (sn)ATAC-seq. We profiled initiating transcripts in two addiction-related brain regions, the prefrontal cortex (PFC) and the nucleus accumbens (NAc), from rats that were never exposed to drugs or were subjected to prolonged abstinence after oxycodone or cocaine intravenous self-administration (IVSA). Interrogating over 100,000 active transcription start regions (TSRs) revealed that most TSRs had hallmarks of bonafide enhancers and highlighted the KLF/SP1, RFX, and AP1 transcription factors families as central to establishing brain-specific gene regulatory programs. Analysis of rats with addiction-like behaviors versus controls identified addiction-associated repression of transcription at regulatory enhancers recognized by nuclear receptor subfamily 3 group C (NR3C) factors, including glucocorticoid receptors. Cell-type deconvolution analysis using snATAC-seq uncovered a potential role of glial cells in driving the gene regulatory programs associated with addiction-related phenotypes. These findings highlight the power of advanced transcriptomics methods to provide insight into how addiction perturbs gene regulatory programs in the brain.

摘要

药物滥用和成瘾是一个重大的公共卫生问题,影响着社会的多个层面,包括医疗保健、经济和劳动力。2021年,美国报告了超过10万例药物过量死亡病例,与阿片类药物和精神兴奋剂相关的死亡人数惊人地增加。了解成瘾及相关行为背后的基本基因调控机制有助于实现更有效的治疗。为了探究反复药物暴露如何改变大脑中的基因调控网络,我们将能够准确从总RNA中捕获新生样起始转录本的带帽小(cs)RNA测序与Hi-C和单核(sn)ATAC测序相结合。我们对从未接触过药物或在羟考酮或可卡因静脉自我给药(IVSA)后经历长期戒断的大鼠的两个与成瘾相关的脑区——前额叶皮层(PFC)和伏隔核(NAc)中的起始转录本进行了分析。对超过10万个活跃转录起始区域(TSR)的研究表明,大多数TSR具有真正增强子的特征,并突出了KLF/SP1、RFX和AP1转录因子家族在建立大脑特异性基因调控程序中的核心作用。对有成瘾样行为的大鼠与对照组的分析确定,在由核受体亚家族3 C组(NR3C)因子(包括糖皮质激素受体)识别的调控增强子处,成瘾会导致转录抑制。使用snATAC测序进行的细胞类型反卷积分析揭示了神经胶质细胞在驱动与成瘾相关表型的基因调控程序中的潜在作用。这些发现凸显了先进转录组学方法在深入了解成瘾如何扰乱大脑基因调控程序方面的强大作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/128f/9149415/73b1323b8ab7/fnins-16-858427-g001.jpg

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