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秀丽隐杆线虫的OSM-11信号在胚胎发育、成虫寿命和应激反应过程中调节SKN-1/Nrf。

Caenorhabditis elegans OSM-11 signaling regulates SKN-1/Nrf during embryonic development and adult longevity and stress response.

作者信息

Dresen Arne, Finkbeiner Sandra, Dottermusch Matthias, Beume Jan-Sebastian, Li Yujie, Walz Gerd, Neumann-Haefelin Elke

机构信息

Department of Medicine, Renal Division, University Hospital Freiburg, D-79106 Freiburg, Germany.

Department of Medicine, Renal Division, University Hospital Freiburg, D-79106 Freiburg, Germany; Center for Biological Signaling Studies (bioss), University of Freiburg, D-79104 Freiburg, Germany.

出版信息

Dev Biol. 2015 Apr 1;400(1):118-31. doi: 10.1016/j.ydbio.2015.01.021. Epub 2015 Jan 29.

Abstract

The Nrf family of transcription factors is critical for stress defense and detoxification. In Caenorhabditis elegans, the Nrf protein ortholog SKN-1 mediates this conserved stress response and promotes longevity. Moreover, SKN-1 is well known for its essential functions during C. elegans embryogenesis. SKN-1 is maternally deployed and initiates a signaling network specifying development of the endoderm and mesoderm. In this study, we identify the conserved Notch ligand OSM-11 as a novel regulator of SKN-1. We find that genetic inactivation of osm-11 re-establishes development of the pharynx and intestine in skn-1 deficient embryos and thereby rescues embryonic lethality associated with loss of skn-1 function. Inactivation of other DSL- and DOS-motif Notch ligands does not prevent skn-1 embryonic lethality. In addition, we show that inactivation of osm-11 in adult worms robustly enhances lifespan and promotes resistance to environmental stress. SKN-1 is required for increased longevity and heat and oxidative stress resistance but not hyperosmotic stress conferred by osm-11. OSM-11 prevents the nuclear accumulation of SKN-1 and represses the transcriptional activation of SKN-1 target genes for cellular detoxification. Our findings indicate that OSM-11 antagonizes SKN-1 during embryonic development and reveal a highly context-specific relationship between OSM-11 and SKN-1 in promoting stress resistance and longevity.

摘要

转录因子Nrf家族对于应激防御和解毒至关重要。在秀丽隐杆线虫中,Nrf蛋白直系同源物SKN-1介导这种保守的应激反应并促进长寿。此外,SKN-1因其在秀丽隐杆线虫胚胎发育过程中的重要功能而闻名。SKN-1由母体传递,并启动一个信号网络来指定内胚层和中胚层的发育。在本研究中,我们鉴定出保守的Notch配体OSM-11是SKN-1的一种新型调节因子。我们发现,osm-11的基因失活可在skn-1缺陷胚胎中重新建立咽部和肠道的发育,从而挽救与skn-1功能丧失相关的胚胎致死性。其他DSL基序和DOS基序Notch配体的失活并不能防止skn-1胚胎致死。此外,我们表明,成年蠕虫中osm-11的失活可显著延长寿命并提高对环境应激的抵抗力。SKN-1是延长寿命以及抵抗热应激和氧化应激所必需的,但不是osm-11所赋予的高渗应激所必需的。OSM-11可阻止SKN-1的核积累,并抑制SKN-1靶基因的转录激活以进行细胞解毒。我们的研究结果表明,OSM-11在胚胎发育过程中拮抗SKN-1,并揭示了OSM-11与SKN-1在促进应激抵抗和长寿方面存在高度上下文特异性的关系。

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