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首页> 外文期刊>Endocrinology >Estradiol regulates corticotropin-releasing hormone gene (crh) expression in a rapid and phasic manner that parallels estrogen receptor-alpha and -beta recruitment to a 3',5'-cyclic adenosine 5'-monophosphate regulatory region of the proximal crh pro
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Estradiol regulates corticotropin-releasing hormone gene (crh) expression in a rapid and phasic manner that parallels estrogen receptor-alpha and -beta recruitment to a 3',5'-cyclic adenosine 5'-monophosphate regulatory region of the proximal crh pro

机译:雌二醇以快速和阶段性的方式调节促肾上腺皮质激素释放激素基因(crh)的表达,使雌激素受体的α和-β募集平行于近端crh pro的3',5'-环腺苷5'-单磷酸调节区域

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In the central nervous system, CRH regulates several affective states. Dysregulation of neuronal crh expression in the paraventricular nucleus of the hypothalamus correlates with some forms of depression, and amygdalar crh expression may modulate levels of anxiety. Because estrogens modulate these states, we sought to determine 17beta-estradiol (E2) effects on crh expression. CRH mRNA levels were measured in the AR-5 amygdaloid cell line by RT-PCR analysis. They increased by 1 min of E2 treatment, suggesting that crh behaves as an immediate-early gene. After peaking at 3 min, CRH mRNA returned to basal levels and then increased by 60 min. To dissect some of the molecular mechanisms underlying these events, we measured occupancy of the crh promoter by estrogen receptors (ERs) and coactivators, using chromatin immunoprecipitation. Because this promoter does not contain palindromic estrogen response elements, we targeted the region of a cAMP regulatory element (CRE), implicated in crh regulation. The temporal pattern of the mRNA response was mimicked by recruitment of ERalpha and -beta, phospho-CRE-binding protein, coactivators steroid receptor coactivator-1 and CRE-binding protein-binding protein (CBP), and an increase in histone 3 and 4 acetylation. Lastly, ERalpha and -beta loading were temporally dissociated, peaking at 1 and 3 min, respectively. The ER peaks were associated with coactivators and acetylation patterns. ERalpha associated with phospho-CRE-binding protein, CBP, steroid receptor coactivator-1, and increased acetylated histone 3. ERbeta associated with CBP and increased acetylated histone 4. The tight temporal correlation between E2-induced CRH mRNA levels and promoter occupancy by ERs strongly suggest that E2 regulates crh expression through an ERalpha- and/or ERbeta-CRE alternate pathway.
机译:在中枢神经系统中,CRH调节几种情感状态。下丘脑室旁核中神经元crh表达的失调与某些形式的抑郁有关,杏仁核crh表达可能调节焦虑水平。因为雌激素调节这些状态,所以我们试图确定17β-雌二醇(E2)对crh表达的影响。通过RT-PCR分析测量AR-5杏仁状细胞系中的CRH mRNA水平。它们在E2处理中增加了1分钟,表明crh表现为早期基因。在3分钟达到峰值后,CRH mRNA恢复至基础水平,然后增加60分钟。为了剖析这些事件背后的某些分子机制,我们使用染色质免疫沉淀法测量了雌激素受体(ER)和共激活因子对crh启动子的占用。因为此启动子不包含回文雌激素反应元件,所以我们靶向cAMP调控元件(CRE)区域,涉及crh调控。通过募集ERalpha和-beta,磷酸CRE结合蛋白,共激活因子类固醇受体共激活因子1和CRE结合蛋白结合蛋白(CBP)以及组蛋白3和4的增加来模仿mRNA反应的时间模式乙酰化。最后,ERalpha和-beta负载在时间上解离,分别在1和3分钟达到峰值。 ER峰与共激活剂和乙酰化模式有关。 ERalpha与磷酸CRE结合蛋白,CBP,类固醇受体共激活因子1相关联,并增加乙酰化组蛋白3。ERbeta与CBP和乙酰化组蛋白4相关。强烈建议E2通过ERalpha和/或ERbeta-CRE替代途径调节crh表达。

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