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血浆生长激素脉冲激活雄性肝脏染色质可及性和STAT5依赖性基因转录

Activation of Male Liver Chromatin Accessibility and STAT5-Dependent Gene Transcription by Plasma Growth Hormone Pulses.

作者信息

Connerney Jeannette, Lau-Corona Dana, Rampersaud Andy, Waxman David J

机构信息

Department of Biology and Bioinformatics Program, Boston University, Boston, Massachusetts 02215.

出版信息

Endocrinology. 2017 May 1;158(5):1386-1405. doi: 10.1210/en.2017-00060.

DOI:10.1210/en.2017-00060
PMID:28323953
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6283433/
Abstract

Sex differences in pituitary growth hormone (GH) secretion (pulsatile in males vs near continuous/persistent in females) impart sex-dependent expression to hundreds of genes in adult mouse liver. Signal transducer and activator of transcription (STAT) 5, a GH-activated transcription factor that is essential for liver sexual dimorphism, is dynamically activated in direct response to each male plasma GH pulse. However, the impact of GH-induced STAT5 pulses on liver chromatin accessibility and downstream transcriptional events is unknown. In this study, we investigated the impact of a single pulse of GH given to hypophysectomized mice on local liver chromatin accessibility (DNase hypersensitive site analysis), transcription rates (heterogeneous nuclear RNA analysis), and gene expression (quantitative polymerase chain reaction and RNA sequencing) determined 30, 90, or 240 minutes later. The STAT5-dependent but sex-independent early GH response genes Igf1 and Cish showed rapid, GH pulse-induced increases in chromatin accessibility and gene transcription, reversing the effects of hypophysectomy. Rapid increases in liver chromatin accessibility and transcriptional activity were also induced in hypophysectomized male mice for some (Ces2b, Ugt2b38) but not for other liver STAT5-dependent male-biased genes (Cyp7b1). Moreover, in pituitary-intact male mice, Igf1, Cish, Ces2b, and Ugt2b38 all showed remarkable cycles of chromatin opening and closing, as well as associated cycles of induced gene transcription, which closely followed each endogenous pulse of liver STAT5 activity. Thus, the endogenous rhythms of male plasma GH pulsation dynamically open and then close liver chromatin at discrete, localized regulatory sites in temporal association with transcriptional activation of Igf1, Cish, and a subset of STAT5-dependent male-biased genes.

摘要

垂体生长激素(GH)分泌的性别差异(雄性为脉冲式分泌,雌性为近乎连续/持续性分泌)使成年小鼠肝脏中数百个基因呈现出性别依赖性表达。信号转导及转录激活因子(STAT)5是一种由GH激活的转录因子,对肝脏的性别二态性至关重要,它会直接响应每一次雄性血浆GH脉冲而动态激活。然而,GH诱导的STAT5脉冲对肝脏染色质可及性和下游转录事件的影响尚不清楚。在本研究中,我们调查了对垂体切除的小鼠给予单次GH脉冲后,在30、90或240分钟后测定的局部肝脏染色质可及性(DNase超敏位点分析)、转录速率(不均一核RNA分析)和基因表达(定量聚合酶链反应和RNA测序)的影响。依赖STAT5但不依赖性别的早期GH反应基因Igf1和Cish显示出染色质可及性和基因转录的快速、GH脉冲诱导增加,逆转了垂体切除的影响。垂体切除的雄性小鼠中,一些肝脏基因(Ces2b、Ugt2b38)的染色质可及性和转录活性也有快速增加,但其他依赖肝脏STAT5的雄性偏向基因(Cyp7b1)则没有。此外,在垂体完整的雄性小鼠中,Igf1、Cish、Ces2b和Ugt2b38均显示出染色质开放和关闭的显著循环,以及相关的诱导基因转录循环,这些循环紧密跟随肝脏STAT5活性的每一次内源性脉冲。因此,雄性血浆GH脉冲的内源性节律在离散的局部调控位点动态地打开然后关闭肝脏染色质,与Igf1、Cish和一部分依赖STAT5的雄性偏向基因的转录激活在时间上相关联。