Direct glucocorticoid receptor-Stat5 interaction in hepatocytes controls body size and maturation-related gene expression.

Engblom D; Kornfeld JW; Schwake L; Tronche F; Reimann A; Beug H; Hennighausen L; Moriggl R; Schutz G

首页> 外文期刊>Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses >Direct glucocorticoid receptor-Stat5 interaction in hepatocytes controls body size and maturation-related gene expression.

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Direct glucocorticoid receptor-Stat5 interaction in hepatocytes controls body size and maturation-related gene expression.

机译：肝细胞中直接糖皮质激素受体与Stat5的相互作用控制着人体大小和与成熟相关的基因表达。

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摘要

The glucocorticoid receptor regulates transcription through DNA binding as well as through cross-talk with other transcription factors. In hepatocytes, the glucocorticoid receptor is critical for normal postnatal growth. Using hepatocyte-specific and domain-selective mutations in the mouse we show that Stat5 in hepatocytes is essential for normal postnatal growth and that it mediates the growth-promoting effect of the glucocorticoid receptor through a direct interaction involving the N-terminal tetramerization domain of Stat5b. This interaction mediates a selective and unexpectedly extensive part of the transcriptional actions of these molecules since it controls the expression of gene sets involved in growth and sexual maturation.

机译：糖皮质激素受体通过DNA结合以及与其他转录因子的串扰来调节转录。在肝细胞中，糖皮质激素受体对于正常的产后生长至关重要。使用小鼠肝细胞特异性和结构域选择性突变，我们表明肝细胞中的Stat5对于正常的出生后生长至关重要，并且它通过涉及Stat5b N端四聚结构域的直接相互作用介导了糖皮质激素受体的促生长作用。。这种相互作用介导了这些分子转录作用的选择性和意想不到的广泛部分，因为它控制着涉及生长和性成熟的基因集的表达。

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《Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses》 |2007年第10期|共6页
作者
Engblom D; Kornfeld JW; Schwake L; Tronche F; Reimann A; Beug H; Hennighausen L; Moriggl R; Schutz G;
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正文语种 eng
中图分类医学遗传学;
关键词
Receptors; Glucocorticoid; SIZES; Direct type of resin cement; postnatal development; 受体; 糖皮质激素;

机译：Receptors;Glucocorticoid;SIZES;Direct type of resin cement;postnatal development;受体;糖皮质激素;

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1. Direct glucocorticoid receptor-Stat5 interaction in hepatocytes controls body size and maturation-related gene expression. [J] . Engblom D, Kornfeld JW, Schwake L, Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses . 2007,第10期

机译：肝细胞中直接糖皮质激素受体与Stat5的相互作用控制着人体大小和与成熟相关的基因表达。
2. Regular article Gastrointestinal, hepatobiliary, and pancreatic pathology Angiocrine Hepatocyte Growth Factor Signaling Controls Physiological Organ and Body Size and Dynamic Hepatocyte Proliferation to Prevent Liver Damage during Regeneration [J] . Xue-jun Zhang, Victor Olsavszky, Yuhan Yin, The American journal of pathology. . 2020,第2期

机译：常规文章胃肠道，肝胆和胰腺病理学血管内肝细胞生长因子信号传导控制生理器官和体尺寸和动态肝细胞增殖，以防止再生过程中的肝脏损伤
3. Generating size-controlled embryoid bodies using laser direct-write [J] . A D Dias, A M Unser, Y Xie, Biofabrication . 2014,第2期

机译：使用激光直接写入生成尺寸受控的类胚体
4. Interactions of Aircraft Design and Control: Actuators Sizing and Optimization for an Unstable Blended Wing-Body [C] . Yann Denieul, Daniel Alazard, Joel Bordeneuve, AIAA atmospheric flight mechanics conference;AIAA SciTech forum . 2015

机译：飞机设计与控制的相互作用：执行器的尺寸调整和不稳定混合机翼机身的优化
5. Measuring dynamic network interactions that control pituitary-gene expression. [D] . Demarco, Ignacio Antonio. 2007

机译：测量控制垂体基因表达的动态网络相互作用。
6. Direct glucocorticoid receptor–Stat5 interaction in hepatocytes controls body size and maturation-related gene expression [O] . David Engblom, Jan-Wilhelm Kornfeld, Lukas Schwake, 2007

机译：肝细胞中糖皮质激素受体–Stat5的直接相互作用控制了体重和与成熟相关的基因表达
7. Direct glucocorticoid receptor–Stat5 interaction in hepatocytes controls body size and maturation-related gene expression [O] . Engblom, David, Kornfeld, Jan-Wilhelm, Schwake, Lukas, 2007

机译：肝细胞中糖皮质激素受体–Stat5的直接相互作用控制了体重和与成熟相关的基因表达

Direct glucocorticoid receptor-Stat5 interaction in hepatocytes controls body size and maturation-related gene expression.

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