中文版 | English
题名

Reciprocal signaling between mTORC1 and MNK2 controls cell growth and oncogenesis

作者
通讯作者Proud,Christopher G.
发表日期
2020
DOI
发表期刊
ISSN
1420-682X
EISSN
1420-9071
摘要
eIF4E plays key roles in protein synthesis and tumorigenesis. It is phosphorylated by the kinases MNK1 and MNK2. Binding of MNKs to eIF4G enhances their ability to phosphorylate eIF4E. Here, we show that mTORC1, a key regulator of mRNA translation and oncogenesis, directly phosphorylates MNK2 on Ser74. This suppresses MNK2 activity and impairs binding of MNK2 to eIF4G. These effects provide a novel mechanism by which mTORC1 signaling impairs the function of MNK2 and thereby decreases eIF4E phosphorylation. MNK2[S74A] knock-in cells show enhanced phosphorylation of eIF4E and S6K1 (i.e., increased mTORC1 signaling), enlarged cell size, and increased invasive and transformative capacities. MNK2[Ser74] phosphorylation was inversely correlated with disease progression in human prostate tumors. MNK inhibition exerted anti-proliferative effects in prostate cancer cells in vitro. These findings define a novel feedback loop whereby mTORC1 represses MNK2 activity and oncogenic signaling through eIF4E phosphorylation, allowing reciprocal regulation of these two oncogenic pathways.
关键词
相关链接[Scopus记录]
收录类别
语种
英语
学校署名
其他
资助项目
Science Foundation for Distinguished Young Scholar of Shanghai, China[2017067] ; Xinglin Scholar Talent Program from Shanghai University of Traditional Chinese Medicine, China[A1-U17205010436] ; Movember Foundation/Prostate Cancer Foundation of Australia[MRTA3] ; Cancer Australia[1138766]
WOS研究方向
Biochemistry & Molecular Biology ; Cell Biology
WOS类目
Biochemistry & Molecular Biology ; Cell Biology
WOS记录号
WOS:000564403700001
出版者
ESI学科分类
MOLECULAR BIOLOGY & GENETICS
Scopus记录号
2-s2.0-85081745513
来源库
Scopus
引用统计
被引频次[WOS]:16
成果类型期刊论文
条目标识符http://sustech.caswiz.com/handle/2SGJ60CL/106417
专题生命科学学院_生物系
生命科学学院
作者单位
1.Lifelong Health Theme,South Australian Health and Medical Research Institute,Adelaide,North Terrace,5000,Australia
2.Medical Research Council Toxicology Unit,Leicester,United Kingdom
3.School of Basic Medical Sciences,Shanghai University of Traditional Chinese Medicine,Shanghai,201203,China
4.Division of Cancer and Genetics,Cardiff University,Heath Park,Cardiff,United Kingdom
5.Adelaide Medical School and Freemasons Foundation Centre for Men’s Health,University of Adelaide,Adelaide,Australia
6.Precision Medicine Theme,South Australian Health and Medical Research Institute,Adelaide,Australia
7.Department of Molecular and Cellular Biology,University of Adelaide,Adelaide,Australia
8.Hopwood Centre for Neurobiology,South Australian Health and Medical Research Institute,Adelaide,Australia
9.Myeloma Research Laboratory,Adelaide Medical School,Faculty of Health and Medical Science,University of Adelaide,Adelaide,Australia
10.Department of Biology,Southern University of Science and Technology,Shenzhen,China
推荐引用方式
GB/T 7714
Xie,Jianling,Shen,Kaikai,Jones,Ashley T.,et al. Reciprocal signaling between mTORC1 and MNK2 controls cell growth and oncogenesis[J]. CELLULAR AND MOLECULAR LIFE SCIENCES,2020.
APA
Xie,Jianling.,Shen,Kaikai.,Jones,Ashley T..,Yang,Jian.,Tee,Andrew R..,...&Proud,Christopher G..(2020).Reciprocal signaling between mTORC1 and MNK2 controls cell growth and oncogenesis.CELLULAR AND MOLECULAR LIFE SCIENCES.
MLA
Xie,Jianling,et al."Reciprocal signaling between mTORC1 and MNK2 controls cell growth and oncogenesis".CELLULAR AND MOLECULAR LIFE SCIENCES (2020).
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