FoxO1-mediated autophagy is required for NK cell development and innate immunity

作者： Wang, Shuo ¹ Xia, Pengyan ¹ Huang, Guanling ¹ Zhu, Pingping ¹ Liu, Jing ¹ Ye, Buqing ¹ Du, Ying ¹ Fan, Zusen ¹ ¹
作者单位：

1. Chinese Acad Sci, Inst Biophys, Key Lab Infect & Immun, Beijing 100101, Peoples R China.
提交时间：2016-05-05 14:39:50

摘要: Natural killer (NK) cells exert a crucial role in early immune responses as a major innate effector component. However, the underlying mechanisms of NK cell development remain largely elusive. Here we show that robust autophagy appears in the stage of immature NK cells (iNKs), which is required for NK cell development. Autophagy defects result in damaged mitochondria and accumulation of reactive oxygen species (ROS) that leads to apoptosis of NK cells. Autophagy protects NK cell viability during development through removal of damaged mitochondria and intracellular ROS. Phosphorylated Forkhead box O (FoxO)1 is located to the cytoplasm of iNKs and interacts with Atg7, leading to induction of autophagy. FoxO1 deficiency or an inactive FoxO1(AAA) mutant abrogates autophagy initiation in iNKs and impairs NK cell development and viral clearance. Therefore we conclude that FoxO1-mediated autophagy is required for NK cell development and NK cell-induced innate immunity.

TRANSCRIPTION FACTOR FOXO1 HEMATOPOIETIC STEM-CELLS NATURAL-KILLER-CELLS LYMPHOID-CELLS IN-VIVO T-BET BONE-MARROW LIFE-SPAN MTOR ACTIVATION

期刊： NATURE COMMUNICATIONS
分类： 生物学 >> 生物物理学
引用： ChinaXiv:201605.00745 (或此版本 ChinaXiv:201605.00745V1)
DOI:10.12074/201605.00745V1
CSTR:32003.36.ChinaXiv.201605.00745.V1
推荐引用方式： Wang, Shuo,Xia, Pengyan,Huang, Guanling,Zhu, Pingping,Liu, Jing,Ye, Buqing,Du, Ying,Fan, Zusen,.(2016).FoxO1-mediated autophagy is required for NK cell development and innate immunity.NATURE COMMUNICATIONS.[ChinaXiv:201605.00745] (点此复制)

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[V1]

2016-05-05 14:39:50

ChinaXiv:201605.00745V1

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