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JNK phosphorylation relieves HDAC3-dependent suppression of the transcriptional activity of c-Jun

机译：JNK磷酸化缓解c-Jun转录活性的HDAC3依赖性抑制

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摘要

The AP-1 transcription factor c-Jun is a prototypical nuclear effector of the JNK signal transduction pathway. The integrity of JNK phosphorylation sites at serines 63/73 and at threonines 91/93 in c-Jun is essential for signal-dependent target gene activation. We show that c-Jun phosphorylation mediates dissociation of an inhibitory complex, which is associated with histone deacetylase 3 (HDAC3). The subsequent events that ultimately cause increased mRNA synthesis are independent of c-Jun phosphorylation and its interaction with JNK. These findings provide an ‘activation by de-repression’ model as an explanation for the stimulatory function of JNK on c-Jun.

机译：AP-1转录因子c-Jun是JNK信号转导途径的典型核效应子。 c-Jun中丝氨酸63/73和苏氨酸91/93的JNK磷酸化位点的完整性对于信号依赖性靶基因激活至关重要。我们表明，c-Jun磷酸化介导与组蛋白脱乙酰基酶3（HDAC3）有关的抑制复合物的解离。最终导致mRNA合成增加的后续事件与c-Jun磷酸化及其与JNK的相互作用无关。这些发现提供了“通过抑制激活”模型，以解释JNK对c-Jun的刺激功能。

著录项

期刊名称 The EMBO Journal
作者
Carsten Weiss; Sandra Schneider; Erwin F. Wagner; Xiaohong Zhang; Edward Seto; Dirk Bohmann;
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作者单位

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年(卷),期 2003(22),14
年度 2003
页码 3686–3695
总页数 10
原文格式 PDF
正文语种
中图分类分子生物学;细胞生物学;
关键词
c-Jun transcription factor/HDAC/MAP kinase/phosphorylation/repression of transcription/signaling;

机译：c-Jun转录因子/ HDAC / MAP激酶/磷酸化/转录抑制/信号转导;

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专利

1. Activity and expression of JNK1, p38 and ERK kinases, c-Jun N-terminal phosphorylation, and c-jun promoter binding in the adult rat brain following kainate-induced seizures. [J] . Mielke K, Brecht S, Dorst A, Neuroscience: An International Journal under the Editorial Direction of IBRO . 1999,第2期

机译：海藻酸盐诱发癫痫发作后成年大鼠脑中JNK1，p38和ERK激酶的活性和表达，c-Jun N末端磷酸化和c-jun启动子结合。
2. Site-specific ubiquitination is required for relieving the transcription factor Miz1-mediated suppression on TNF-α-induced JNK activation and inflammation [J] . Jing Liu, Jie Yari, Shan Jiang, Proceedings of the National Academy of Sciences of the United States of America . 2012,第1期

机译：需要位点特异性泛素化来减轻转录因子Miz1介导的对TNF-α诱导的JNK激活和炎症的抑制
3. Impaired dynamin 2 function leads to increased AP-1 transcriptional activity through the JNK/c-Jun pathway [J] . Szymanska Ewelina, Skowronek Agnieszka, Miaczynska Marta Cellular Signalling . 2016,第1期

机译：动力蛋白2功能受损导致通过JNK / c-Jun途径增加AP-1转录活性
4. Particulate Joint Replacement Materials Induce Apoptosis of Rabbit Synoviocytes Cell Line HIG-82 through c-Jun N-Terminal Kinase (JNK) Pathway [C] . Chu Feng-Min, Lian Shuang-Shii, Sung Yen-Jen International Conference on Biomedical Engineering and Informatics;BMEI '09 . 2009

机译：颗粒关节替代材料通过c-Jun N末端激酶（JNK）途径诱导兔滑膜细胞HIG-82细胞凋亡
5. Nicotine and learning interact to alter transcription factor activity at the c-Jun N-terminal kinase 1 gene promoter in the hippocampus. [D] . Kenney, Justin W. 2010

机译：尼古丁和学习相互作用以改变海马c-Jun N端激酶1基因启动子的转录因子活性。
6. Site-specific ubiquitination is required for relieving the transcription factor Miz1-mediated suppression on TNF-α–induced JNK activation and inflammation [O] . Jing Liu, Jie Yan, Shan Jiang, 2012

机译：需要位点特异性泛素化来减轻转录因子Miz1介导的对TNF-α诱导的JNK激活和炎症的抑制
7. JNK phosphorylation relieves HDAC3-dependent suppression of the transcriptional activity of c-Jun [O] . C. Weiss 2003

机译：JNK磷酸化可缓解HDAC3依赖性抑制C-Jun的转录活动

JNK phosphorylation relieves HDAC3-dependent suppression of the transcriptional activity of c-Jun

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