Rint1 inactivation triggers genomic instability, ER stress and autophagy inhibition in the brain

Grigaravicius P.; Kaminska E.; Huebner C. A.; McKinnon P. J.; von Deimling A.; Frappart P-O

首页> 外文期刊>Cell death and differentiation >Rint1 inactivation triggers genomic instability, ER stress and autophagy inhibition in the brain

【24h】

Rint1 inactivation triggers genomic instability, ER stress and autophagy inhibition in the brain

机译：Rint1失活触发基因组不稳定，内质网应激和自噬抑制

获取原文

获取原文并翻译 | 示例

掌桥外文数据库（机构版） >>

开具论文收录证明 >>

页面导航

摘要
著录项
相似文献
相关主题

摘要

Endoplasmic reticulum (ER) stress, defective autophagy and genomic instability in the central nervous system are often associated with severe developmental defects and neurodegeneration. Here, we reveal the role played by Rint1 in these different biological pathways to ensure normal development of the central nervous system and to prevent neurodegeneration. We found that inactivation of Rint1 in neuroprogenitors led to death at birth. Depletion of Rint1 caused genomic instability due to chromosome fusion in dividing cells. Furthermore, Rint1 deletion in developing brain promotes the disruption of ER and Cis/Trans Golgi homeostasis in neurons, followed by ER-stress increase. Interestingly, Rint1 deficiency was also associated with the inhibition of the autophagosome clearance. Altogether, our findings highlight the crucial roles of Rint1 in vivo in genomic stability maintenance, as well as in prevention of ER stress and autophagy.

机译：内质网（ER）应力，自噬缺陷和中枢神经系统基因组不稳定通常与严重的发育缺陷和神经变性相关。在这里，我们揭示了Rint1在这些不同的生物学途径中所起的作用，以确保中枢神经系统的正常发育并防止神经退行性变。我们发现神经祖细胞中Rint1的失活导致出生时死亡。由于分裂细胞中的染色体融合，Rint1的耗尽导致基因组不稳定。此外，发育中的大脑中的Rint1缺失促进神经元内质网和顺式/反式高尔基体内稳态的破坏，随后内质网应激增加。有趣的是，Rint1缺乏也与自噬体清除的抑制有关。总而言之，我们的发现突出了Rint1在体内在基因组稳定性维持以及预防ER应激和自噬中的关键作用。

著录项

来源
《Cell death and differentiation》 |2016年第3期|共15页
作者
Grigaravicius P.; Kaminska E.; Huebner C. A.; McKinnon P. J.; von Deimling A.; Frappart P-O;
展开▼
作者单位

展开▼
收录信息
原文格式 PDF
正文语种 eng
中图分类细胞生物学;
关键词
入库时间 2022-08-18 09:19:51

相似文献

外文文献
中文文献
专利

1. Rint1 inactivation triggers genomic instability, ER stress and autophagy inhibition in the brain [J] . Grigaravicius P., Kaminska E., Huebner C. A., Cell death and differentiation . 2016,第3期

机译：Rint1失活触发基因组不稳定，内质网应激和自噬抑制
2. RINT1 functions as a multitasking protein at the crossroads between genomic stability, ER homeostasis, and autophagy [J] . Grigaravicius Paulius, von Deimling Andreas, Frappart Pierre-Olivier Autophagy . 2016,第8期

机译：RINT1在基因组稳定性，ER稳态和自噬之间的十字路口时用作多任务蛋白
3. Selection of autophagy or apoptosis in cells exposed to ER-stress depends on ATF4 expression pattern with or without CHOP expression Selection of autophagy or apoptosis in cells exposed to ER-stress depends on ATF4 expression pattern with or without CHOP expression Selection of autophagy or apoptosis in cells exposed to ER-stress depends on ATF4 expression pattern with or without CHOP expression [J] . Hiroki Matsumoto, Satoshi Matsuyama, Hiroshi Nakagawa, Biology Open . 2013,第10期

机译：暴露于内质网应激的细胞中自噬或凋亡的选择取决于有或没有CHOP表达的ATF4表达模式选择有内质网应激的细胞中自噬或凋亡的选择取决于有或没有CHOP表达的ATF4表达模式暴露于内质网应激的细胞取决于有无CHOP表达的ATF4表达模式
4. Arsenic trioxide induces both apoptosis and autophagy through stimulation of ER stress and inhibition of ubiquitin-proteasome system in human sarcoma cells [C] . H.-W. Chiu, Y.-C. Tseng, Y.-J. Wang International Congress on Arsenic in the Environment . 2014

机译：通过刺激人类肉瘤细胞中的ER应激和泛素 - 蛋白酶体系的ER应激和抑制来诱导细胞凋亡和自噬
5. Rint1 inactivation triggers genomic instability ER stress and autophagy inhibition in the brain [O] . P Grigaravicius, E Kaminska, C A Hübner, 2016

机译：Rint1失活会触发基因组不稳定内质网应激和自噬抑制
6. Inhibition of CLIC4 Enhances Autophagy and Triggers Mitochondrial and ER Stress-Induced Apoptosis in Human Glioma U251 Cells under Starvation [O] . Zhong, Jiateng, Kong, Xiaoxia, Zhang, Hongyu, 2012

机译：在饥饿状态下抑制CLIC4增强自噬并触发线粒体和ER应激诱导的人胶质瘤U251细胞凋亡。

Rint1 inactivation triggers genomic instability, ER stress and autophagy inhibition in the brain

摘要

著录项

相似文献

相关主题

期刊订阅