MicroRNAs recruit eIF4E2 to repress translation of target mRNAs
TNRC6A
0303 health sciences
QH573-671
RNA-Binding Proteins
QP501-801
Autoantigens
Animal biochemistry
microRNAs
Cell Line
5′ cap
MicroRNAs
Protein Transport
03 medical and health sciences
Eukaryotic Initiation Factor-4E
Humans
Gene Silencing
RNA, Messenger
translation repression
Cytology
eIF4E2
Research Article
DOI:
10.1007/s13238-017-0444-0
Publication Date:
2017-07-28T11:02:57Z
AUTHORS (2)
ABSTRACT
MicroRNAs (miRNAs) recruit the RNA-induced silencing complex (RISC) to repress the translation of target mRNAs. While the 5' 7-methylguanosine cap of target mRNAs has been well known to be important for miRNA repression, the underlying mechanism is not clear. Here we show that TNRC6A interacts with eIF4E2, a homologue of eIF4E that can bind to the cap but cannot interact with eIF4G to initiate translation, to inhibit the translation of target mRNAs. Downregulation of eIF4E2 relieved miRNA repression of reporter expression. Moreover, eIF4E2 downregulation increased the protein levels of endogenous IMP1, PTEN and PDCD4, whose expression are repressed by endogenous miRNAs. We further provide evidence showing that miRNA enhances eIF4E2 association with the target mRNA. We propose that miRNAs recruit eIF4E2 to compete with eIF4E to repress mRNA translation.
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